Diels–Alder Cycloaddition Reactions in Sustainable Media

Diels–Alder cycloaddition reaction is one of the most powerful strategies for the construction of six-membered carbocyclic and heterocyclic systems, in most cases with high regio- and stereoselectivity. In this review, an insight into the most relevant advances on sustainable Diels–Alder reactions since 2010 is provided. Various environmentally benign solvent systems are discussed, namely bio-based derived solvents (such as glycerol and gluconic acid), polyethylene glycol, deep eutectic solvents, supercritical carbon dioxide, water and water-based aqueous systems. Issues such as method’s scope, efficiency, selectivity and reaction mechanism, as well as sustainability, advantages and limitations of these reaction media, are addressed.


Introduction
The Diels-Alder reaction, a concerted [4 + 2] cycloaddition of a conjugated diene and a dienophile, is a powerful tool for the regio-and stereoselective construction of six-membered rings [1][2][3][4][5][6]. In its original version, two new C-C bonds are created in the Diels-Alder reaction and six-membered carbocyclic systems are obtained. Beyond this classical Diels-Alder reaction, other well-known types include the hetero-Diels-Alder reaction (at least one heteroatom is present on the diene or dienophile) leading to sixmembered heterocycles and the intramolecular Diels-Alder reaction in which fused cyclic systems are obtained. Additionally, the Lewis acid catalyzed and organocatalytic Diels-Alder reactions have been developed, widening the scope of these reactions, namely the synthesis of optically active compounds via catalyzed asymmetric Diels-Alder reactions. Notably, a century after its discovery, the Diels-Alder reaction remains one of the most important green synthetic methodologies due to its theoretical 100% atom economy [7].

Gluconic Acid
Gluconic acid (GA) can be obtained from biomass and possesses the ideal properties for being classified as a green and sustainable solvent (e.g., nontoxicity, biodegradability, recyclability, high boiling point, low vapor pressure) [51]. Due to the high solubility of gluconic acid in water, gluconic acid aqueous solutions (GAASs) have found wide application as solvent media for organic reactions, namely for the Knoevenagel condensation reaction. The Gu group reported the synthesis of 2H-pyrans by a one-pot multicomponent reaction between β-ketosulfones, formaldehyde and styrenes in a biobased binary mixture solvent system composed of GAAS and a sugar-based organic base, meglumine [52]. The disclosed protocol involves the in situ generation of α-methylene-βketosulfones 21 through a Knoevenagel reaction of β-ketosulfones 19 and formaldehyde. Next, nucleophilic trap of 21 with styrenes 22 via oxa-Diels-Alder reaction afforded 2,6diaryl-5-(phenylsulfonyl)-3,4-dihydro-2H-pyrans 23 in moderate to good yields (50-82%) (Scheme 5). The binary solvent system GAAS/meglumine proved to play a pivotal role in controlling the selectivity of the hydroxymethylation step. Moreover, the hydrophilic properties of bio-based solvent meglumine allowed it to be easily recycled and reused in the GAAS/meglumine system without significant loss of activity.

Polyethylene Glycol
Polyethylene glycol (PEG), HO-(CH 2 CH 2 O) n -H, is a biodegradable, nontoxic, odorless, neutral, nonvolatile and inexpensive water-soluble polymer that has found widespread application as a green reaction medium for several organic transformations [20]. The Kouznetsov group reported the diastereoselective synthesis of heterolignan-like 6,7methylendioxy-tetrahydroquinolines via a BF 3 . OEt-catalyzed three-component Povarov reaction using clove bud essential oil as a renewable raw material and PEG-400 as green solvent (Scheme 6) [53]. Clove bud essential oil enriched with eugenol 24 (60.5%) was obtained by hydrodistillation of dried flower buds and then subjected to a solid basecatalyzed isomerization to give trans/cis-isoeugenol 25, which could be used as a dienophile in the multicomponent hetero-Diels-Alder reaction without further purification. The reaction of 25 with aldimines generated in situ from substituted benzaldehydes 27 and 3,4-(methylendioxy)aniline (26) afforded trans-2,4-diaryl-1,2,3,4-tetrahydroquinolines 28 as racemic mixtures in moderate yields (35-55%). The reaction with phthalaldehydic acid (29) afforded isoindolo[2,1-a]quinolin-11(5H)-one 30 via an intramolecular condensation of the initially generated NH-tetrahydroquinoline core with the o-carboxylic acid function leading to the formation of the γ-lactam ring. It is noteworthy that these reactions also worked using acetonitrile as solvent media; however, less solvent volume and reduced reaction times were required when using PEG-400.
The intramolecular Povarov reaction of 2-aminoarylaldehydes bearing a tethered alkyne moiety with heterocyclic amines catalyzed by Amberlyst-15 in PEG-200 has been described [54]. This metal-free green protocol allowed the synthesis of [1,6]-naphthyridinefused heterocycles 33 and 35 in good yields (60-81%) starting from 2-(N-propargylamino)-arylaldehydes 31 and 3-aminocoumarins 32 or 3-methyl-1-aryl-1H-pyrazol-5-amines 34, respectively (Scheme 7). The synthesis of these heterocyclic systems involves the initial formation of imine intermediate 36, followed by an Amberlyst-15 promoted intramolecular [4 + 2] hetero Diels-Alder reaction as the key step. Deprotonation followed by air oxidation afforded the final products. It is worth mentioning the high atom economy of the protocol (over 96%) since water is the only by-product, as well as the use of an eco-friendly solvent and a recyclable catalyst. propargylamino)-arylaldehydes 31 and 3-aminocoumarins 32 or 3-methyl-1-aryl-1Hpyrazol-5-amines 34, respectively (Scheme 7). The synthesis of these heterocyclic systems involves the initial formation of imine intermediate 36, followed by an Amberlyst-15 promoted intramolecular [4 + 2] hetero Diels-Alder reaction as the key step. Deprotonation followed by air oxidation afforded the final products. It is worth mentioning the high atom economy of the protocol (over 96%) since water is the only byproduct, as well as the use of an eco-friendly solvent and a recyclable catalyst. Chandrasekhar and coworkers described the Diels-Alder reaction of cyclopentadiene (39) with substituted cinnamaldehydes 40, catalyzed by (S)-TMSdiphenylprolinol (41) using PEG-400 as solvent (Scheme 8) [55]. It was demonstrated that the endo/exo selectivity of the cycloaddition can be controlled by the addition of an acid cocatalyst which favors the formation of the endo-adduct. Thus, the reaction of cyclopentadiene (39) with cinnamaldehydes 40 in the presence of 41 as organocatalyst and perchloric acid as cocatalyst gave selectively endo-cycloadducts 42 as major products. The observed diastereoselectivity was rationalized by considering the involvement of the enamine complex intermediate 44 which was formed from cinnamaldehyde and the proline-derived organocatalyst and then enclosed in PEG-400 and stabilized by perchloric acid. The authors suggested that the cavity-like arrangement of the complex may be responsible for the facial selectivity which leads to the preferential formation of the endocycloadduct. Scheme 8. Diels-Alder reaction of cyclopentadiene and substituted cinnamaldehydes in PEG-400 catalyzed by a TMS-diphenylprolinol/perchloric acid catalytic system.
Chandrasekhar and coworkers described the Diels-Alder reaction of cyclopentadiene (39) with substituted cinnamaldehydes 40, catalyzed by (S)-TMS-diphenylprolinol (41) using PEG-400 as solvent (Scheme 8) [55]. It was demonstrated that the endo/exo selectivity of the cycloaddition can be controlled by the addition of an acid cocatalyst which favors the formation of the endo-adduct. Thus, the reaction of cyclopentadiene (39) with cinnamaldehydes 40 in the presence of 41 as organocatalyst and perchloric acid as cocatalyst gave selectively endo-cycloadducts 42 as major products. The observed diastereoselectivity was rationalized by considering the involvement of the enamine complex intermediate 44 which was formed from cinnamaldehyde and the proline-derived organocatalyst and then enclosed in PEG-400 and stabilized by perchloric acid. The authors suggested that the cavity-like arrangement of the complex may be responsible for the facial selectivity which leads to the preferential formation of the endo-cycloadduct. propargylamino)-arylaldehydes 31 and 3-aminocoumarins 32 or 3-methyl-1-aryl-1Hpyrazol-5-amines 34, respectively (Scheme 7). The synthesis of these heterocyclic systems involves the initial formation of imine intermediate 36, followed by an Amberlyst-15 promoted intramolecular [4 + 2] hetero Diels-Alder reaction as the key step. Deprotonation followed by air oxidation afforded the final products. It is worth mentioning the high atom economy of the protocol (over 96%) since water is the only byproduct, as well as the use of an eco-friendly solvent and a recyclable catalyst. Chandrasekhar and coworkers described the Diels-Alder reaction of cyclopentadiene (39) with substituted cinnamaldehydes 40, catalyzed by (S)-TMSdiphenylprolinol (41) using PEG-400 as solvent (Scheme 8) [55]. It was demonstrated that the endo/exo selectivity of the cycloaddition can be controlled by the addition of an acid cocatalyst which favors the formation of the endo-adduct. Thus, the reaction of cyclopentadiene (39) with cinnamaldehydes 40 in the presence of 41 as organocatalyst and perchloric acid as cocatalyst gave selectively endo-cycloadducts 42 as major products. The observed diastereoselectivity was rationalized by considering the involvement of the enamine complex intermediate 44 which was formed from cinnamaldehyde and the proline-derived organocatalyst and then enclosed in PEG-400 and stabilized by perchloric acid. The authors suggested that the cavity-like arrangement of the complex may be responsible for the facial selectivity which leads to the preferential formation of the endocycloadduct. Scheme 8. Diels-Alder reaction of cyclopentadiene and substituted cinnamaldehydes in PEG-400 catalyzed by a TMS-diphenylprolinol/perchloric acid catalytic system.

Organic Carbonates
Propylene carbonate (PC) is a polar aprotic solvent that can be obtained from propylene oxide and carbon dioxide, a renewable source of carbon, in a 100% atom economy reaction with relevance regarding the development of CO 2 fixation processes. The noncorrosive, nontoxic, odorless and biodegradable properties of PC, allied with high boiling point, low vapor pressure and low cost, make this solvent a green and sustainable alternative to conventional organic solvents [56]. The Povarov reaction has also been explored using PC as an environmentally friendly solvent [57]. The one-pot iodine-catalyzed reaction of monoor disubstituted anilines 2, aromatic aldehydes 5 and isoeugenol (45) carried out at room temperature using PC as solvent medium afforded functionalized tetrahydroquinolines 46 in good to high yields (77-95%) and high diastereoselectivity (dr up to >99:1) (Scheme 9). The same cycloadducts were obtained using organic solvents (e.g., dichloromethane, acetonitrile, toluene), albeit in low yields and requiring longer reaction times. It is noteworthy that, in general, products precipitated from the reaction medium and were purified by recrystallization.

Organic Carbonates
Propylene carbonate (PC) is a polar aprotic solvent that can be obtained from propylene oxide and carbon dioxide, a renewable source of carbon, in a 100% atom economy reaction with relevance regarding the development of CO2 fixation processes. The noncorrosive, nontoxic, odorless and biodegradable properties of PC, allied with high boiling point, low vapor pressure and low cost, make this solvent a green and sustainable alternative to conventional organic solvents [56]. The Povarov reaction has also been explored using PC as an environmentally friendly solvent [57]. The one-pot iodinecatalyzed reaction of mono-or disubstituted anilines 2, aromatic aldehydes 5 and isoeugenol (45) carried out at room temperature using PC as solvent medium afforded functionalized tetrahydroquinolines 46 in good to high yields (77-95%) and high diastereoselectivity (dr up to >99:1) (Scheme 9). The same cycloadducts were obtained using organic solvents (e.g., dichloromethane, acetonitrile, toluene), albeit in low yields and requiring longer reaction times. It is noteworthy that, in general, products precipitated from the reaction medium and were purified by recrystallization. Scheme 9. Iodine-catalyzed one-pot multicomponent aza-Diels-Alder reaction of anilines, aromatic aldehydes and isoeugenol in propylene carbonate.
Dimethyl carbonate (DMC) is a nontoxic methylating and/or methoxycarbonylating agent with wide application in the sustainable valorization of renewables [58,59]. Like PC, DMC can be synthesized by a green process using CO2 as a building block and can also be used as an eco-friendly solvent in several organic transformations. Ollevier and coworkers reported the Diels-Alder reaction of α,β-unsaturated carbonyl and Nacyloxazolidinone derivatives 47 with cyclopentadiene (39) using DMC as a green solvent (Scheme 10) [60]. Among the solvents tested, from conventional organic solvents (dichloromethane and THF) to greener solvents (e.g., N-methylpyrrolidone, cyclopentyl methyl ether), DMC proved to be the most selective, affording cycloadducts with the highest yields and endo/exo ratio. Thus, the reaction of diene 39 and dienophiles 47, catalyzed by the recyclable iron(II) caffeine-derived ionic salt 48 and carried out in DMC, afforded cycloadducts 49 and 50 in good yields (up to 99%) and endo-selectivity. The reaction was also carried out in cyclohexa-1,3-diene; however, a longer reaction time was needed and the corresponding cycloadducts were obtained in low overall yield (20%) and 77:23 endo/exo ratio. Dimethyl carbonate (DMC) is a nontoxic methylating and/or methoxycarbonylating agent with wide application in the sustainable valorization of renewables [58,59]. Like PC, DMC can be synthesized by a green process using CO 2 as a building block and can also be used as an eco-friendly solvent in several organic transformations. Ollevier and coworkers reported the Diels-Alder reaction of α,β-unsaturated carbonyl and N-acyloxazolidinone derivatives 47 with cyclopentadiene (39) using DMC as a green solvent (Scheme 10) [60]. Among the solvents tested, from conventional organic solvents (dichloromethane and THF) to greener solvents (e.g., N-methylpyrrolidone, cyclopentyl methyl ether), DMC proved to be the most selective, affording cycloadducts with the highest yields and endo/exo ratio. Thus, the reaction of diene 39 and dienophiles 47, catalyzed by the recyclable iron(II) caffeine-derived ionic salt 48 and carried out in DMC, afforded cycloadducts 49 and 50 in good yields (up to 99%) and endo-selectivity. The reaction was also carried out in cyclohexa-1,3-diene; however, a longer reaction time was needed and the corresponding cycloadducts were obtained in low overall yield (20%) and 77:23 endo/exo ratio.

Deep Eutectic Solvents
First introduced by Abbot [61], deep eutectic solvents (DESs) are low melting mixtures obtained by combination of at least two components, a hydrogen bond acceptor (HBA), generally a quaternary ammonium or metal salt, and a hydrogen bond donor (HBD), to form a eutectic phase via hydrogen bond interactions. DESs are characterized by a melting point lower than those of the single components. The properties of DESs are very similar to those of room-temperature ionic liquids; however, the main difference from ionic liquids is that DESs also contain an organic molecular component, the HBD (e.g., urea, amide, polyol), generally as a major component. Due to their low vapor pressure, nonflammability, thermal and chemical stability, nontoxicity, biodegradability, recyclability and low price, DESs have emerged as green and sustainable media in different areas of chemical research [62][63][64][65], namely organic synthesis and catalysis [23][24][25][26].
In 2011, Nagare and Kumare reported a kinetic study of the Diels-Alder reaction between cyclopentadiene (39) and methyl acrylate (51a) using binary mixtures of urea, or methylated urea (DMU), with carbohydrates, or ternary mixtures of urea derivatives, NH4Cl and carbohydrates, demonstrating the potential of these eutectic mixtures as solvent media to accelerate this bimolecular reaction (Scheme 11) [66]. They observed that the experimental rate constants were dependent on the percentage of urea in the carbohydrate melt; however, the best correlation was found to be with the solvent viscosity, which is in agreement with previous reports by the authors [67]. Scheme 11. Diels-Alder reaction of cyclopentadiene with methyl acrylate in carbohydrate-ureasalt eutectic melts, including kinetic and solvent viscosity data.
The Diels-Alder reaction of 9-anthracenemethanol (54) and N-ethylmaleimide (55a) in different solvent media under conventional heating and ultrasonic activation has been reported [68]. The influence of the solvent medium in the yield of the reaction was assessed by comparing DESs, obtained by the combination of different HBAs (e.g., choline chloride, methyltriphenylphosphonium chloride, (±)-menthol) and HBDs (e.g., glycerol (Gly), ethylene glycol (EG), urea), with water and organic solvents. In general, the Diels-Alder reaction of 54 and 55a proved to be more efficient when carried out in eutectic Scheme 10. Diels-Alder reaction of cyclopentadiene and α,β-unsaturated carbonyls in dimethyl carbonate catalyzed by an iron(II) caffeine-derived ionic salt.

Deep Eutectic Solvents
First introduced by Abbot [61], deep eutectic solvents (DESs) are low melting mixtures obtained by combination of at least two components, a hydrogen bond acceptor (HBA), generally a quaternary ammonium or metal salt, and a hydrogen bond donor (HBD), to form a eutectic phase via hydrogen bond interactions. DESs are characterized by a melting point lower than those of the single components. The properties of DESs are very similar to those of room-temperature ionic liquids; however, the main difference from ionic liquids is that DESs also contain an organic molecular component, the HBD (e.g., urea, amide, polyol), generally as a major component. Due to their low vapor pressure, nonflammability, thermal and chemical stability, nontoxicity, biodegradability, recyclability and low price, DESs have emerged as green and sustainable media in different areas of chemical research [62][63][64][65], namely organic synthesis and catalysis [23][24][25][26].
In 2011, Nagare and Kumare reported a kinetic study of the Diels-Alder reaction between cyclopentadiene (39) and methyl acrylate (51a) using binary mixtures of urea, or methylated urea (DMU), with carbohydrates, or ternary mixtures of urea derivatives, NH 4 Cl and carbohydrates, demonstrating the potential of these eutectic mixtures as solvent media to accelerate this bimolecular reaction (Scheme 11) [66]. They observed that the experimental rate constants were dependent on the percentage of urea in the carbohydrate melt; however, the best correlation was found to be with the solvent viscosity, which is in agreement with previous reports by the authors [67].

Deep Eutectic Solvents
First introduced by Abbot [61], deep eutectic solvents (DESs) are low melting mixtures obtained by combination of at least two components, a hydrogen bond acceptor (HBA), generally a quaternary ammonium or metal salt, and a hydrogen bond donor (HBD), to form a eutectic phase via hydrogen bond interactions. DESs are characterized by a melting point lower than those of the single components. The properties of DESs are very similar to those of room-temperature ionic liquids; however, the main difference from ionic liquids is that DESs also contain an organic molecular component, the HBD (e.g., urea, amide, polyol), generally as a major component. Due to their low vapor pressure, nonflammability, thermal and chemical stability, nontoxicity, biodegradability, recyclability and low price, DESs have emerged as green and sustainable media in different areas of chemical research [62][63][64][65], namely organic synthesis and catalysis [23][24][25][26].
In 2011, Nagare and Kumare reported a kinetic study of the Diels-Alder reaction between cyclopentadiene (39) and methyl acrylate (51a) using binary mixtures of urea, or methylated urea (DMU), with carbohydrates, or ternary mixtures of urea derivatives, NH4Cl and carbohydrates, demonstrating the potential of these eutectic mixtures as solvent media to accelerate this bimolecular reaction (Scheme 11) [66]. They observed that the experimental rate constants were dependent on the percentage of urea in the carbohydrate melt; however, the best correlation was found to be with the solvent viscosity, which is in agreement with previous reports by the authors [67]. Scheme 11. Diels-Alder reaction of cyclopentadiene with methyl acrylate in carbohydrate-ureasalt eutectic melts, including kinetic and solvent viscosity data.
The Diels-Alder reaction of 9-anthracenemethanol (54) and N-ethylmaleimide (55a) in different solvent media under conventional heating and ultrasonic activation has been reported [68]. The influence of the solvent medium in the yield of the reaction was assessed by comparing DESs, obtained by the combination of different HBAs (e.g., choline chloride, methyltriphenylphosphonium chloride, (±)-menthol) and HBDs (e.g., glycerol (Gly), ethylene glycol (EG), urea), with water and organic solvents. In general, the Diels-Alder reaction of 54 and 55a proved to be more efficient when carried out in eutectic Scheme 11. Diels-Alder reaction of cyclopentadiene with methyl acrylate in carbohydrate-urea-salt eutectic melts, including kinetic and solvent viscosity data.
The Diels-Alder reaction of 9-anthracenemethanol (54) and N-ethylmaleimide (55a) in different solvent media under conventional heating and ultrasonic activation has been reported [68]. The influence of the solvent medium in the yield of the reaction was assessed by comparing DESs, obtained by the combination of different HBAs (e.g., choline chloride, methyltriphenylphosphonium chloride, (±)-menthol) and HBDs (e.g., glycerol (Gly), ethylene glycol (EG), urea), with water and organic solvents. In general, the Diels-Alder reaction of 54 and 55a proved to be more efficient when carried out in eutectic mixtures than in conventional solvents (Scheme 12). Moreover, it has been demonstrated that DESs could be recycled up to eight times without yield decrease and that the reaction time can be reduced from 24 h to 70 min when carrying out the reaction under ultrasound irradiation. The activating effect of DESs was attributed to the combined action of solvent viscosity, polarity and structure. The effect of bio-based DESs on the endo/exo ratio of the Diels-Alder reaction of cyclopentadiene (39) and acrylates 51 has been recently described (Scheme 13) [69]. DESs, prepared from racemic and optically enriched HBAs obtained from crude glycerol, proved to be more effective than organic solvents or ionic liquids, allowing cycloadducts to be obtained in higher yields and selectivity. The higher yields and endo-selectivity were achieved using lactic acid (LA) as the HBD of the eutectic mixture. However, a direct relationship between the chiral environment of the solvent and the observed selectivity was not demonstrated. It is noteworthy that cycloadducts were isolated from the reaction mixture by simple extraction with diethyl ether. Garcia-Álvarez's group reported a one-pot tandem cycloisomerization/Diels-Alder reaction using a ChCl (choline chloride)-based eutectic mixture as solvent [70]. The protocol involves the in situ generation of furans 59 by cycloisomerization of (Z)-enynols 57 using a ChCl/Gly (1:2) eutectic mixture as solvent and bis(iminophosphorane)-Au(I) complex 58 as catalyst (Scheme 14). The Diels-Alder reaction of furans 59 with activated alkynes 60 afforded 7-oxanorbornadienes 61, whereas the reaction with activated alkenes, 55b or 62, afforded selectively exo-7-oxanorbornenes 63. The authors have demonstrated that complex 58 is crucial for the cycloisomerization step; however, it does not participate in the cycloaddition step.  The effect of bio-based DESs on the endo/exo ratio of the Diels-Alder reaction of cyclopentadiene (39) and acrylates 51 has been recently described (Scheme 13) [69]. DESs, prepared from racemic and optically enriched HBAs obtained from crude glycerol, proved to be more effective than organic solvents or ionic liquids, allowing cycloadducts to be obtained in higher yields and selectivity. The higher yields and endo-selectivity were achieved using lactic acid (LA) as the HBD of the eutectic mixture. However, a direct relationship between the chiral environment of the solvent and the observed selectivity was not demonstrated. It is noteworthy that cycloadducts were isolated from the reaction mixture by simple extraction with diethyl ether. The effect of bio-based DESs on the endo/exo ratio of the Diels-Alder reaction of cyclopentadiene (39) and acrylates 51 has been recently described (Scheme 13) [69]. DESs, prepared from racemic and optically enriched HBAs obtained from crude glycerol, proved to be more effective than organic solvents or ionic liquids, allowing cycloadducts to be obtained in higher yields and selectivity. The higher yields and endo-selectivity were achieved using lactic acid (LA) as the HBD of the eutectic mixture. However, a direct relationship between the chiral environment of the solvent and the observed selectivity was not demonstrated. It is noteworthy that cycloadducts were isolated from the reaction mixture by simple extraction with diethyl ether. Garcia-Álvarez's group reported a one-pot tandem cycloisomerization/Diels-Alder reaction using a ChCl (choline chloride)-based eutectic mixture as solvent [70]. The protocol involves the in situ generation of furans 59 by cycloisomerization of (Z)-enynols 57 using a ChCl/Gly (1:2) eutectic mixture as solvent and bis(iminophosphorane)-Au(I) complex 58 as catalyst (Scheme 14). The Diels-Alder reaction of furans 59 with activated alkynes 60 afforded 7-oxanorbornadienes 61, whereas the reaction with activated alkenes, 55b or 62, afforded selectively exo-7-oxanorbornenes 63. The authors have demonstrated that complex 58 is crucial for the cycloisomerization step; however, it does not participate in the cycloaddition step.  Garcia-Álvarez's group reported a one-pot tandem cycloisomerization/Diels-Alder reaction using a ChCl (choline chloride)-based eutectic mixture as solvent [70]. The protocol involves the in situ generation of furans 59 by cycloisomerization of (Z)-enynols 57 using a ChCl/Gly (1:2) eutectic mixture as solvent and bis(iminophosphorane)-Au(I) complex 58 as catalyst (Scheme 14). The Diels-Alder reaction of furans 59 with activated alkynes 60 afforded 7-oxanorbornadienes 61, whereas the reaction with activated alkenes, 55b or 62, afforded selectively exo-7-oxanorbornenes 63. The authors have demonstrated that complex 58 is crucial for the cycloisomerization step; however, it does not participate in the cycloaddition step. Molecules 2022, 27, x FOR PEER REVIEW 10 of 47 Scheme 14. One-pot tandem cycloisomerization/Diels-Alder reaction of (Z)-enynols in a ChCl/Gly deep eutectic solvent.
The synthesis of 3,5-dimethylcyclohex-4-ene-1,2-dicarboxylates using a ChCl-based DES medium has been reported [71]. The methodology involves a Raney Ni-catalyzed hydrogenation of diacetone alcohol 64 followed by a one-step dehydration/Diels-Alder reaction of the resulting 2-methylpentane-2,4-diol 65 and diethyl fumarate (67) in a ChCl/EG deep eutectic mixture, catalyzed by Amberlyst-15, leading to the formation of compound 68 as a single product (Scheme 15). Mechanistic studies demonstrated that the ChCl/EG and Amberlyst-15 play a role in the dehydration of 65, affording 1,3-dienes 66a and 66b as a mixture (1:1.5). The observed selectivity was rationalized considering that the Diels-Alder reaction between 67 and 66b is faster than that between 67 and 66a, shifting the equilibrium from 66a to 66b and favoring the exclusive formation of 68. Compound 68 and analogous derivatives could be further hydrogenated to give compounds that can serve as safe plasticizers for PVC materials. Owing to their high reactivity and versatility, nitrosoalkenes and azoalkenes have been extensively used as building blocks for the synthesis and functionalization of an array of heterocycles. These electron-deficient heterodienes participate in inverse electron demand hetero-Diels-Alder reactions with a wide range of electron-rich heterocycles and nucleophilic olefins [72].
Pinho e Melo and coworkers disclosed the first example of an inverse electron demand hetero-Diels-Alder reaction in natural DESs [73]. Oxime-and hydrazonebis(indolyl)methanes (BIMs) 71 were obtained as single Z-isomers via one-pot bis-hetero-Diels-Alder reaction of nitrosoalkenes and azoalkenes with indoles using a ternary mixture of water with ChCl/Gly (Scheme 16). The protocol allowed the synthesis of BIMs in a more efficient and sustainable way than the previously reported strategies using DCM or a water/DCM solvent system [74,75]. The proposed mechanism involves the in situ generation of nitrosoalkenes or azoalkenes 73 by base-mediated dehydrohalogenation of α,α-dihalooximes or α,α-dihalohydrazones 69, respectively, followed by hetero-Diels-Alder reaction with indoles to give cycloadducts 74. Rearomatization of the indole unit triggers ring-opening of the six-membered ring affording 3-alkylindoles 75 bearing an α-Scheme 14. One-pot tandem cycloisomerization/Diels-Alder reaction of (Z)-enynols in a ChCl/Gly deep eutectic solvent.
The synthesis of 3,5-dimethylcyclohex-4-ene-1,2-dicarboxylates using a ChCl-based DES medium has been reported [71]. The methodology involves a Raney Ni-catalyzed hydrogenation of diacetone alcohol 64 followed by a one-step dehydration/Diels-Alder reaction of the resulting 2-methylpentane-2,4-diol 65 and diethyl fumarate (67) in a ChCl/EG deep eutectic mixture, catalyzed by Amberlyst-15, leading to the formation of compound 68 as a single product (Scheme 15). Mechanistic studies demonstrated that the ChCl/EG and Amberlyst-15 play a role in the dehydration of 65, affording 1,3-dienes 66a and 66b as a mixture (1:1.5). The observed selectivity was rationalized considering that the Diels-Alder reaction between 67 and 66b is faster than that between 67 and 66a, shifting the equilibrium from 66a to 66b and favoring the exclusive formation of 68. Compound 68 and analogous derivatives could be further hydrogenated to give compounds that can serve as safe plasticizers for PVC materials. The synthesis of 3,5-dimethylcyclohex-4-ene-1,2-dicarboxylates using a ChCl-based DES medium has been reported [71]. The methodology involves a Raney Ni-catalyzed hydrogenation of diacetone alcohol 64 followed by a one-step dehydration/Diels-Alder reaction of the resulting 2-methylpentane-2,4-diol 65 and diethyl fumarate (67) in a ChCl/EG deep eutectic mixture, catalyzed by Amberlyst-15, leading to the formation of compound 68 as a single product (Scheme 15). Mechanistic studies demonstrated that the ChCl/EG and Amberlyst-15 play a role in the dehydration of 65, affording 1,3-dienes 66a and 66b as a mixture (1:1.5). The observed selectivity was rationalized considering that the Diels-Alder reaction between 67 and 66b is faster than that between 67 and 66a, shifting the equilibrium from 66a to 66b and favoring the exclusive formation of 68. Compound 68 and analogous derivatives could be further hydrogenated to give compounds that can serve as safe plasticizers for PVC materials. Owing to their high reactivity and versatility, nitrosoalkenes and azoalkenes have been extensively used as building blocks for the synthesis and functionalization of an array of heterocycles. These electron-deficient heterodienes participate in inverse electron demand hetero-Diels-Alder reactions with a wide range of electron-rich heterocycles and nucleophilic olefins [72].
Pinho e Melo and coworkers disclosed the first example of an inverse electron demand hetero-Diels-Alder reaction in natural DESs [73]. Oxime-and hydrazonebis(indolyl)methanes (BIMs) 71 were obtained as single Z-isomers via one-pot bis-hetero-Diels-Alder reaction of nitrosoalkenes and azoalkenes with indoles using a ternary mixture of water with ChCl/Gly (Scheme 16). The protocol allowed the synthesis of BIMs in a more efficient and sustainable way than the previously reported strategies using DCM or a water/DCM solvent system [74,75]. The proposed mechanism involves the in situ generation of nitrosoalkenes or azoalkenes 73 by base-mediated dehydrohalogenation of α,α-dihalooximes or α,α-dihalohydrazones 69, respectively, followed by hetero-Diels-Alder reaction with indoles to give cycloadducts 74. Rearomatization of the indole unit triggers ring-opening of the six-membered ring affording 3-alkylindoles 75 bearing an α-Scheme 15. One-step dehydration/Diels-Alder reaction of 2-methylpentane-2,4-diol and diethyl fumarate in a ChCl/EG deep eutectic solvent.
Owing to their high reactivity and versatility, nitrosoalkenes and azoalkenes have been extensively used as building blocks for the synthesis and functionalization of an array of heterocycles. These electron-deficient heterodienes participate in inverse electron demand hetero-Diels-Alder reactions with a wide range of electron-rich heterocycles and nucleophilic olefins [72].
Pinho e Melo and coworkers disclosed the first example of an inverse electron demand hetero-Diels-Alder reaction in natural DESs [73]. Oxime-and hydrazone-bis(indolyl) methanes (BIMs) 71 were obtained as single Z-isomers via one-pot bis-hetero-Diels-Alder reaction of nitrosoalkenes and azoalkenes with indoles using a ternary mixture of water with ChCl/Gly (Scheme 16). The protocol allowed the synthesis of BIMs in a more efficient and sustainable way than the previously reported strategies using DCM or a water/DCM solvent system [74,75]. The proposed mechanism involves the in situ generation of nitrosoalkenes or azoalkenes 73 by base-mediated dehydrohalogenation of α,α-dihalooximes or α,α-dihalohydrazones 69, respectively, followed by hetero-Diels-Alder reaction with indoles to give cycloadducts 74. Rearomatization of the indole unit triggers ring-opening of the six-membered ring affording 3-alkylindoles 75 bearing an α-halogenated oxime or hydrazone at the side chain. Dehydrohalogenation of 75 generates the corresponding 3-alkylheterodienes which react with another indole molecule, at the s-cis conformation, via a second hetero-Diels-Alder reaction to give BIMs 71 as single Z-isomers. In some cases, the formation of E/Z-isomeric mixtures of 71 resulting from an alternative mechanistic pathway via conjugated addition reactions was observed. When longer reaction times were used, carbonyl-BIMs 72 were obtained via a one-pot tandem hetero-Diels-Alder or conjugate addition/hydrolysis sequence. halogenated oxime or hydrazone at the side chain. Dehydrohalogenation of 75 generates the corresponding 3-alkylheterodienes which react with another indole molecule, at the s-cis conformation, via a second hetero-Diels-Alder reaction to give BIMs 71 as single Zisomers. In some cases, the formation of E/Z-isomeric mixtures of 71 resulting from an alternative mechanistic pathway via conjugated addition reactions was observed. When longer reaction times were used, carbonyl-BIMs 72 were obtained via a one-pot tandem hetero-Diels-Alder or conjugate addition/hydrolysis sequence. Scheme 16. One-pot tandem bis-hetero-Diels-Alder/conjugate addition reactions of nitroso-and azoalkenes with indoles in a ternary mixture of water with ChCl/Gly.
Ochoa-Puentes and coworkers explored the multicomponent Povarov reaction for the one-pot synthesis of quinoline derivatives using zinc chloride based eutectic mixtures as reaction media [76,77]. Tetrahydroquinolines 77 were obtained with endo-selectively by the reaction of trans-anethole (76), the major component of star anise oil obtained by hydrodistillation of anise seeds, with anilines 2 and aromatic aldehydes 5 using a ChCl/ZnCl2 eutectic mixture (Scheme 17a) [76]. On the other hand, the reaction of anilines 2, aromatic aldehydes 5 and indene (78) performed in a urea/ZnCl2 eutectic mixture led to the synthesis of indeno[2,1-c]quinolines 79 in high yields (89-99%) (Scheme 17b) [77]. The proposed mechanism for the formation of quinolines involves the initial reaction of amine 2 with DES-activated aldehyde to give N-aryl imine (Schiff's base) 80 followed by DES activation to generate intermediate 81.
The endo-selectivity could be rationalized considering that 81 participates in a [4 + 2] concerted cycloaddition via a trans-endofavored transition state followed by a 1,3-H shift. However, the most plausible mechanism was rationalized considering a two-step ionic mechanism involving an endo-selective nucleophilic dienophile attack to imine 81 followed by an intramolecular Friedel-Crafts reaction to give selectively the 2,4-cis-isomer 77. In the formation of indenoquinolines 79 an additional aerobic oxidative dehydrogenation was proposed. It is noteworthy that for both synthetic procedures, DESs were reused up to three cycles and green metric analysis demonstrated that the synthetic strategy has a favorable environmental impact. Scheme 16. One-pot tandem bis-hetero-Diels-Alder/conjugate addition reactions of nitroso-and azoalkenes with indoles in a ternary mixture of water with ChCl/Gly. Ochoa-Puentes and coworkers explored the multicomponent Povarov reaction for the one-pot synthesis of quinoline derivatives using zinc chloride based eutectic mixtures as reaction media [76,77]. Tetrahydroquinolines 77 were obtained with endo-selectively by the reaction of trans-anethole (76), the major component of star anise oil obtained by hydrodistillation of anise seeds, with anilines 2 and aromatic aldehydes 5 using a ChCl/ZnCl 2 eutectic mixture (Scheme 17a) [76]. On the other hand, the reaction of anilines 2, aromatic aldehydes 5 and indene (78) performed in a urea/ZnCl 2 eutectic mixture led to the synthesis of indeno[2,1-c]quinolines 79 in high yields (89-99%) (Scheme 17b) [77]. The proposed mechanism for the formation of quinolines involves the initial reaction of amine 2 with DES-activated aldehyde to give N-aryl imine (Schiff's base) 80 followed by DES activation to generate intermediate 81.
The endo-selectivity could be rationalized considering that 81 participates in a [4 + 2] concerted cycloaddition via a trans-endo-favored transition state followed by a 1,3-H shift. However, the most plausible mechanism was rationalized considering a two-step ionic mechanism involving an endo-selective nucleophilic dienophile attack to imine 81 followed by an intramolecular Friedel-Crafts reaction to give selectively the 2,4-cis-isomer 77. In the formation of indenoquinolines 79 an additional aerobic oxidative dehydrogenation was proposed. It is noteworthy that for both synthetic procedures, DESs were reused up to three cycles and green metric analysis demonstrated that the synthetic strategy has a favorable environmental impact. DESs have also been successfully employed as environmentally friendly reaction media for the covalent functionalization of carbon nanomaterials via catalyst-free Diels-Alder click reaction. In 2018, Lim's group reported the functionalization of multiwalled carbon nanotubes (MWNTs) with polymeric materials containing ionic liquids (ILs) in their repeating units [78]. The Diels-Alder reaction of MWNTs 83 and imidazolium-based poly(ionic liquid)s featuring furfuryl moieties (P(F-ILs)) 84 was performed in a Ch/EG eutectic mixture under ultrasound irradiation at 60 °C (Scheme 18). Functionalized MWNTs 85 were obtained with shorter reaction times and higher grafting density of P(F-ILs) on MWNTs when compared with the reaction in water. Recently, the same strategy was applied for the covalent functionalization of reduced graphene oxide (rGO) with P(F-ILs), delivering a new rGO-P(F-IL) hybrid material with good electrochemical capacitor behavior [79]. DESs have also been successfully employed as environmentally friendly reaction media for the covalent functionalization of carbon nanomaterials via catalyst-free Diels-Alder click reaction. In 2018, Lim's group reported the functionalization of multiwalled carbon nanotubes (MWNTs) with polymeric materials containing ionic liquids (ILs) in their repeating units [78]. The Diels-Alder reaction of MWNTs 83 and imidazolium-based poly(ionic liquid)s featuring furfuryl moieties (P(F-ILs)) 84 was performed in a Ch/EG eutectic mixture under ultrasound irradiation at 60 • C (Scheme 18). Functionalized MWNTs 85 were obtained with shorter reaction times and higher grafting density of P(F-ILs) on MWNTs when compared with the reaction in water. Recently, the same strategy was applied for the covalent functionalization of reduced graphene oxide (rGO) with P(F-ILs), delivering a new rGO-P(F-IL) hybrid material with good electrochemical capacitor behavior [79].

Supercritical Carbon Dioxide
Supercritical carbon dioxide (scCO2) is an abundant, low-cost, nontoxic and nonflammable fluid. The physical properties of scCO2 are intermediate between the gas and the liquid phases. These properties can be tuned by changing pressure and temperature; in particular, changes close to the critical point enable drastic changes in density, viscosity and diffusion. Among supercritical fluids (SCFs), scCO2 has received special attention since it is readily accessible at a low critical temperature (Tc = 31 °C) and moderate critical pressure (Pc = 75.8 bar) [80,81]. In addition, scCO2 has the ability to dissolve organic compounds and can be easily removed from the reaction mixture, making it a sustainable alternative to conventional organic solvents in synthetic transformations [27][28][29][30][31]. Keshtov et al. disclosed a green approach for the synthesis of photoluminescent polymers based on phenyl-substituted polyfluorenes using scCO2 as the solvent medium [82]. Phenylated polyfluorenes 88 were synthesized through a catalyst-free Diels-Alder reaction of fluorene-containing bis(tetraarylcyclopentadienone) monomer 86, acting as diene, with bis(acetylenes) 87 acting as 2π-component (Scheme 19). Phenyl-substituted polyfluorenes synthesized using scCO2 as solvent showed similar properties to those synthesized using chloronaphthalene as solvent, demonstrating that scCO2 is a suitable alternative to organic solvents for the synthesis of phenylated polyfluorenes via the Diels-Alder reaction.

Supercritical Carbon Dioxide
Supercritical carbon dioxide (scCO 2 ) is an abundant, low-cost, nontoxic and nonflammable fluid. The physical properties of scCO 2 are intermediate between the gas and the liquid phases. These properties can be tuned by changing pressure and temperature; in particular, changes close to the critical point enable drastic changes in density, viscosity and diffusion. Among supercritical fluids (SCFs), scCO 2 has received special attention since it is readily accessible at a low critical temperature (T c = 31 • C) and moderate critical pressure (P c = 75.8 bar) [80,81]. In addition, scCO 2 has the ability to dissolve organic compounds and can be easily removed from the reaction mixture, making it a sustainable alternative to conventional organic solvents in synthetic transformations [27][28][29][30][31]. Keshtov et al. disclosed a green approach for the synthesis of photoluminescent polymers based on phenyl-substituted polyfluorenes using scCO 2 as the solvent medium [82]. Phenylated polyfluorenes 88 were synthesized through a catalyst-free Diels-Alder reaction of fluorene-containing bis(tetraarylcyclopentadienone) monomer 86, acting as diene, with bis(acetylenes) 87 acting as 2π-component (Scheme 19). Phenyl-substituted polyfluorenes synthesized using scCO 2 as solvent showed similar properties to those synthesized using chloronaphthalene as solvent, demonstrating that scCO 2 is a suitable alternative to organic solvents for the synthesis of phenylated polyfluorenes via the Diels-Alder reaction.

Supercritical Carbon Dioxide
Supercritical carbon dioxide (scCO2) is an abundant, low-cost, nontoxic and nonflammable fluid. The physical properties of scCO2 are intermediate between the gas and the liquid phases. These properties can be tuned by changing pressure and temperature; in particular, changes close to the critical point enable drastic changes in density, viscosity and diffusion. Among supercritical fluids (SCFs), scCO2 has received special attention since it is readily accessible at a low critical temperature (Tc = 31 °C) and moderate critical pressure (Pc = 75.8 bar) [80,81]. In addition, scCO2 has the ability to dissolve organic compounds and can be easily removed from the reaction mixture, making it a sustainable alternative to conventional organic solvents in synthetic transformations [27][28][29][30][31]. Keshtov et al. disclosed a green approach for the synthesis of photoluminescent polymers based on phenyl-substituted polyfluorenes using scCO2 as the solvent medium [82]. Phenylated polyfluorenes 88 were synthesized through a catalyst-free Diels-Alder reaction of fluorene-containing bis(tetraarylcyclopentadienone) monomer 86, acting as diene, with bis(acetylenes) 87 acting as 2π-component (Scheme 19). Phenyl-substituted polyfluorenes synthesized using scCO2 as solvent showed similar properties to those synthesized using chloronaphthalene as solvent, demonstrating that scCO2 is a suitable alternative to organic solvents for the synthesis of phenylated polyfluorenes via the Diels-Alder reaction. The Diels-Alder reaction of cyclopentadiene (39) and 1,3-butadiene (89) in scCO 2 has been reported, allowing the synthesis of 5-vinyl-2-norbornene 90, a precursor of 5ethylidene-2-norbornene which is a valuable monomer used in the manufacture of ethylene propylene rubber (Scheme 20) [83]. The major drawback of this reaction is the reactivity pattern of the starting materials, cyclopentadiene and 1,3-butadiene, that can act as both dienes and dienophiles in the Diels-Alder reaction and therefore give rise to a panoply of by-products (e.g., 91). The Diels-Alder reaction of 39 and 89 was carried out in neat conditions, in the presence of organic solvents and in scCO 2 . The most satisfactory yields and selectivities were achieved when using scCO 2 as the solvent medium, providing the target compound 90 in 25% yield, by-product 91 in 17% yield and other unidentified compounds in 6% yield. The observed slight increase in selectivity was rationalized considering the unique physical properties of scCO 2 acting as a thinner and allowing the suppression of eventual side reactions, being an alternative to the commonly used large amounts of solvents and/or inhibitors. ethylidene-2-norbornene which is a valuable monomer used in the manufacture of ethylene propylene rubber (Scheme 20) [83]. The major drawback of this reaction is the reactivity pattern of the starting materials, cyclopentadiene and 1,3-butadiene, that can act as both dienes and dienophiles in the Diels-Alder reaction and therefore give rise to a panoply of by-products (e.g., 91). The Diels-Alder reaction of 39 and 89 was carried out in neat conditions, in the presence of organic solvents and in scCO2. The most satisfactory yields and selectivities were achieved when using scCO2 as the solvent medium, providing the target compound 90 in 25% yield, by-product 91 in 17% yield and other unidentified compounds in 6% yield. The observed slight increase in selectivity was rationalized considering the unique physical properties of scCO2 acting as a thinner and allowing the suppression of eventual side reactions, being an alternative to the commonly used large amounts of solvents and/or inhibitors.
Ito and coworkers disclosed a protocol for the synthesis of isoindoles from bicyclopyrroles by a retro-Diels-Alder reaction in scCO2 [84]. In general, bicyclopyrroles were converted into the corresponding isoindoles in high yields; however, in some cases, the instability associated with the exomethylenic structure causes the decomposition of the isoindole derivatives. In these cases, the formation of the retro-Diels-Alder product in the reaction medium was confirmed by performing the retro-Diels-Alder reaction in the presence of a trapping agent for isoindole. Thus, the reaction of N-tosylated bicyclopyrrole 92 in the presence of N-phenylmaleimide (55c) carried out in scCO2 (20 MPa) at 185 °C over 210 min led to the formation of the exo-Diels-Alder adduct 94 in 72% yield, which confirms the generation of isoindole 93 under the reaction conditions (Scheme 21). Scheme 21. Diels-Alder reaction of N-tosyl-isoindole and N-phenylmaleimide in scCO2.

Water
The use of water as an alternative benign and sustainable solvent in promoting Diels-Alder cycloaddition reactions has been widely explored since the seminal work of Breslow's and Grieco's groups [85][86][87][88]. The remarkable rate enhancements and selectivities achieved on moving from conventional organic solvents to aqueous conditions are the major driving force behind the growing interest in the study of the Diels-Alder reaction in this medium [37,38].

The Water Effect: Experimental and Theoretical Studies
Hydrophobic interactions, along with hydrogen bonding, polarity and cohesive energy density, are the major factors responsible for the rate enhancement in "on-water" Diels-Alder cycloadditions. Several systematic experimental and theoretical studies analyzing the pivotal role of water in the rate enhancement and selectivity of the Diels-Scheme 20. Diels-Alder reaction of cyclopentadiene and 1,3-butadiene carried out in organic solvents and scCO 2 .
Ito and coworkers disclosed a protocol for the synthesis of isoindoles from bicyclopyrroles by a retro-Diels-Alder reaction in scCO 2 [84]. In general, bicyclopyrroles were converted into the corresponding isoindoles in high yields; however, in some cases, the instability associated with the exomethylenic structure causes the decomposition of the isoindole derivatives. In these cases, the formation of the retro-Diels-Alder product in the reaction medium was confirmed by performing the retro-Diels-Alder reaction in the presence of a trapping agent for isoindole. Thus, the reaction of N-tosylated bicyclopyrrole 92 in the presence of N-phenylmaleimide (55c) carried out in scCO 2 (20 MPa) at 185 • C over 210 min led to the formation of the exo-Diels-Alder adduct 94 in 72% yield, which confirms the generation of isoindole 93 under the reaction conditions (Scheme 21). ethylidene-2-norbornene which is a valuable monomer used in the manufacture of ethylene propylene rubber (Scheme 20) [83]. The major drawback of this reaction is the reactivity pattern of the starting materials, cyclopentadiene and 1,3-butadiene, that can act as both dienes and dienophiles in the Diels-Alder reaction and therefore give rise to a panoply of by-products (e.g., 91). The Diels-Alder reaction of 39 and 89 was carried out in neat conditions, in the presence of organic solvents and in scCO2. The most satisfactory yields and selectivities were achieved when using scCO2 as the solvent medium, providing the target compound 90 in 25% yield, by-product 91 in 17% yield and other unidentified compounds in 6% yield. The observed slight increase in selectivity was rationalized considering the unique physical properties of scCO2 acting as a thinner and allowing the suppression of eventual side reactions, being an alternative to the commonly used large amounts of solvents and/or inhibitors.
Ito and coworkers disclosed a protocol for the synthesis of isoindoles from bicyclopyrroles by a retro-Diels-Alder reaction in scCO2 [84]. In general, bicyclopyrroles were converted into the corresponding isoindoles in high yields; however, in some cases, the instability associated with the exomethylenic structure causes the decomposition of the isoindole derivatives. In these cases, the formation of the retro-Diels-Alder product in the reaction medium was confirmed by performing the retro-Diels-Alder reaction in the presence of a trapping agent for isoindole. Thus, the reaction of N-tosylated bicyclopyrrole 92 in the presence of N-phenylmaleimide (55c) carried out in scCO2 (20 MPa) at 185 °C over 210 min led to the formation of the exo-Diels-Alder adduct 94 in 72% yield, which confirms the generation of isoindole 93 under the reaction conditions (Scheme 21). Scheme 21. Diels-Alder reaction of N-tosyl-isoindole and N-phenylmaleimide in scCO2.

Water
The use of water as an alternative benign and sustainable solvent in promoting Diels-Alder cycloaddition reactions has been widely explored since the seminal work of Breslow's and Grieco's groups [85][86][87][88]. The remarkable rate enhancements and selectivities achieved on moving from conventional organic solvents to aqueous conditions are the major driving force behind the growing interest in the study of the Diels-Alder reaction in this medium [37,38].

The Water Effect: Experimental and Theoretical Studies
Hydrophobic interactions, along with hydrogen bonding, polarity and cohesive energy density, are the major factors responsible for the rate enhancement in "on-water" Diels-Alder cycloadditions. Several systematic experimental and theoretical studies analyzing the pivotal role of water in the rate enhancement and selectivity of the Diels-Scheme 21. Diels-Alder reaction of N-tosyl-isoindole and N-phenylmaleimide in scCO 2 .

Water
The use of water as an alternative benign and sustainable solvent in promoting Diels-Alder cycloaddition reactions has been widely explored since the seminal work of Breslow's and Grieco's groups [85][86][87][88]. The remarkable rate enhancements and selectivities achieved on moving from conventional organic solvents to aqueous conditions are the major driving force behind the growing interest in the study of the Diels-Alder reaction in this medium [37,38].

The Water Effect: Experimental and Theoretical Studies
Hydrophobic interactions, along with hydrogen bonding, polarity and cohesive energy density, are the major factors responsible for the rate enhancement in "on-water" Diels-Alder cycloadditions. Several systematic experimental and theoretical studies analyzing the pivotal role of water in the rate enhancement and selectivity of the Diels-Alder cycloaddition reactions have been disclosed. Shrinidhi reported a comparative study of the rates and efficiency of the Diels-Alder cycloaddition reaction between cyclopentadiene (39) and electron-poor alkenes 95 in solvent media featuring different polarities (organic solvents and water) (Scheme 22) [89]. For each dienophile, it was observed that cycloadducts 96 yield increases with the increase in solvent polarity (hexane < dichloromethane < THFwater < water) and concomitantly with the solvophilicity of the dienophile. The effect of adding a catalytic amount of water along with organic solvents (dichloromethane and THF) was also explored, demonstrating that the reaction is more efficient in the presence of catalytic amounts of water than in pure organic solvents. Based on these results, combined hydrophobic and hydrogen bonding effects were attributed to the rate enhancement of the Diels-Alder reaction when carried out in water as compared to conventional organic solvents. The hydrogen bonding effect was previously reported by Domingo's group supported by a density functional theory (DFT) study on the catalytic effect of water in the intramolecular Diels-Alder reaction of a quinone system [90]. Theoretical calculations demonstrated the pivotal role of water in stabilizing the polarized transition state through hydrogen bond formation with the internal electron-deficient dienophile. Alder cycloaddition reactions have been disclosed. Shrinidhi reported a comparative study of the rates and efficiency of the Diels-Alder cycloaddition reaction between cyclopentadiene (39) and electron-poor alkenes 95 in solvent media featuring different polarities (organic solvents and water) (Scheme 22) [89]. For each dienophile, it was observed that cycloadducts 96 yield increases with the increase in solvent polarity (hexane < dichloromethane < THF-water < water) and concomitantly with the solvophilicity of the dienophile. The effect of adding a catalytic amount of water along with organic solvents (dichloromethane and THF) was also explored, demonstrating that the reaction is more efficient in the presence of catalytic amounts of water than in pure organic solvents. Based on these results, combined hydrophobic and hydrogen bonding effects were attributed to the rate enhancement of the Diels-Alder reaction when carried out in water as compared to conventional organic solvents. The hydrogen bonding effect was previously reported by Domingo's group supported by a density functional theory (DFT) study on the catalytic effect of water in the intramolecular Diels-Alder reaction of a quinone system [90]. Theoretical calculations demonstrated the pivotal role of water in stabilizing the polarized transition state through hydrogen bond formation with the internal electrondeficient dienophile. The Vilches-Herrera group reported an experimental and theoretical study on the influence of noncovalent interactions in the stereo-and regioselectivity of the aza-Diels-Alder reaction between 5-aminopyrrole-derived aldimines and electron-poor dienophiles [91]. Depending on the nature of substituents present on both diene and dienophile, the reaction of aldimines 97 and electron-poor styryl substrates 98, carried out in water under MW irradiation over 20 min, afforded regio-and stereoselectively the exo-adducts of tetrahydro-1H-pyrrolo[2,3-b]pyridines 99, or 7-azaindoles 100, also in a regioselective fashion (Scheme 23). The reaction is also compatible with alkynes (dimethyl acetylenedicarboxylate) and monosubstituted alkenes (ethyl acrylate and acrylonitrile); however, in the latter case, mixtures of regioisomers were obtained. The experimental results were corroborated by DFT calculations which suggest that the regioselectivity and the unusual exo-selectivity were controlled by noncovalent attractive π-π interactions at the TS region instead of secondary orbital interactions. In the absence of noncovalent interactions (e.g., with ethyl acrylate), thermodynamic control prevails and regioisomeric mixtures were obtained. The Vilches-Herrera group reported an experimental and theoretical study on the influence of noncovalent interactions in the stereo-and regioselectivity of the aza-Diels-Alder reaction between 5-aminopyrrole-derived aldimines and electron-poor dienophiles [91]. Depending on the nature of substituents present on both diene and dienophile, the reaction of aldimines 97 and electron-poor styryl substrates 98, carried out in water under MW irradiation over 20 min, afforded regio-and stereoselectively the exo-adducts of tetrahydro-1H-pyrrolo[2,3-b]pyridines 99, or 7-azaindoles 100, also in a regioselective fashion (Scheme 23). The reaction is also compatible with alkynes (dimethyl acetylenedicarboxylate) and monosubstituted alkenes (ethyl acrylate and acrylonitrile); however, in the latter case, mixtures of regioisomers were obtained. The experimental results were corroborated by DFT calculations which suggest that the regioselectivity and the unusual exo-selectivity were controlled by noncovalent attractive π-π interactions at the TS region instead of secondary orbital interactions. In the absence of noncovalent interactions (e.g., with ethyl acrylate), thermodynamic control prevails and regioisomeric mixtures were obtained. A comparative study on the rates of the Diels-Alder reaction of 9hydroxymethylanthracene (54) and N-phenylmaleimide (55c) in water, ethylene glycol and conventional organic solvents (butan-1-ol, acetonitrile, chloroform and 1,4-dioxane) has been reported (Scheme 24) [92]. Kinetic measurements, performed at 45 °C using spectrophotometric methods, showed that, under homogeneous conditions, no relevant The kinetics of the Diels-Alder cycloaddition reactions in water can be modified by the presence of inorganic salts, which can change the hydrophobic interactions involving the diene and dienophile, the internal pressure (by changing the cohesive energy) and the solvation of the transition states. The Kumar group studied the influence of quaternary ammonium salts in the cycloaddition of 9-hydroxymethylanthracene (54) and Nethylmaleimide (55a) in water, concluding that higher concentrations of salt in the reaction media lead to a deceleration of the reaction rate [93]. This was rationalized by the reduction in hydrophobic interactions, responsible for bringing the reactants closer, which were progressively blocked upon the continuous increase in the concentration of salt. They also concluded that ammonium salts bearing long alkyl groups promote the dissolution of the nonpolar reactants by rearranging water molecules up to a second solvation shell around the dissolved salts, thus behaving as anti-hydrophobic or saltingin agents. In another study, Shimizu and coworkers investigated the effect of several rateenhancing salts (e.g., LiCl, guanidinium sulfate) and rate-reducing salts (e.g., NaClO4, guanidinium acetate) for the same reaction, demonstrating that the interactions between ions and diene 54 are crucial for controlling the reaction rate [94]. A rate reduction was observed for the reaction in the presence of rate-reducing salts, which show a preferential interaction with diene, and is consistent with the increased 54 solubility. On the other hand, the major driving force behind the rate enhancement with rate-enhancing salts is the salting-out of the hydrophobic diene 54 by the rate-enhancing salt, which exhibits a stronger affinity with the transition state. The effect of LiCl on the Diels-Alder reaction of Scheme 24. Kinetic data for the Diels-Alder reaction of 9-hydroxymethylanthracene and Nphenylmaleimide in different solvents.
The kinetics of the Diels-Alder cycloaddition reactions in water can be modified by the presence of inorganic salts, which can change the hydrophobic interactions involving the diene and dienophile, the internal pressure (by changing the cohesive energy) and the solvation of the transition states. The Kumar group studied the influence of quaternary ammonium salts in the cycloaddition of 9-hydroxymethylanthracene (54) and N-ethylmaleimide (55a) in water, concluding that higher concentrations of salt in the reaction media lead to a deceleration of the reaction rate [93]. This was rationalized by the reduction in hydrophobic interactions, responsible for bringing the reactants closer, which were progressively blocked upon the continuous increase in the concentration of salt. They also concluded that ammonium salts bearing long alkyl groups promote the dissolution of the nonpolar reactants by rearranging water molecules up to a second solvation shell around the dissolved salts, thus behaving as anti-hydrophobic or salting-in agents. In another study, Shimizu and coworkers investigated the effect of several rate-enhancing salts (e.g., LiCl, guanidinium sulfate) and rate-reducing salts (e.g., NaClO 4 , guanidinium acetate) for the same reaction, demonstrating that the interactions between ions and diene 54 are crucial for controlling the reaction rate [94]. A rate reduction was observed for the reaction in the presence of rate-reducing salts, which show a preferential interaction with diene, and is consistent with the increased 54 solubility. On the other hand, the major driving force behind the rate enhancement with rate-enhancing salts is the salting-out of the hydrophobic diene 54 by the rate-enhancing salt, which exhibits a stronger affinity with the transition state. The effect of LiCl on the Diels-Alder reaction of cyclopentadiene (39) and methyl vinyl ketone in water was also investigated, demonstrating a rate enhancement in the presence of this salt arising from the destabilization of the reactants by hydrophobic effect resulting in the decrease in the activation barrier [95]. The instability associated with the hydrophobic interaction in the transition state complexes is suppressed by the formation of hydrogen bonds, which are stronger compared to those of the dienophile.
Kumar and coworkers reported a Diels-Alder cycloaddition reaction of cyclopentadiene (39) with methyl acrylate (51a) using a recyclable and highly viscous supersaturated water-based solvent obtained by supersaturation of water (~18% w/w) with carbohydrates, an organic acid and an organic ketone [96]. The second-order rate constant (k 2 , 7.92 × 10 −5 M −1 s −1 ) determined for the reaction carried at room temperature is about 26-fold higher than that obtained for the same reaction in water. This rate enhancement was attributed to the combined presence of OH groups from the carbohydrates, which allows multiple hydrogen bonding sites, and the hydrophobic effect by water molecules.
It is noteworthy that it is also possible to carry out the reaction of cyclopentadiene (39) and methyl acrylate (51a) using eutectic mixtures of carbohydrates as solvent medium; however, to ensure these mixtures were in a liquid state, higher temperatures (>85 • C) were required (cf. Scheme 11) [66,96].

Noncatalyzed Diels-Alder Cycloaddition Reactions
Romám and coworkers reported a catalyst-free protocol for the Diels-Alder cycloaddition of water-insoluble furan derivatives and N-substituted maleimides using "on-water" conditions [97]. The reaction of furans 102 and maleimides 55 carried out at room temperature afforded cycloadducts 103 and 104 in quantitative yields and endo-selectivity (Scheme 25a). When the reaction was carried out at 65 • C, the reaction times were shortened and an increase in the exo-adducts was observed. On the other hand, the reaction between furfural N,N-dimethylhydrazone (105) and maleimides 55 afforded selectively the exo-adducts 106 obtained as single products, mixtures of 106 and phthalimides 107, or 107 as the sole products, depending on the maleimide precursors and reaction conditions (Scheme 25b). Upon heating, cycloadducts 106 can be converted into the corresponding phthalimides 107, whose formation was rationalized considering the ring-opening of the exo-7-oxabicycle followed by dehydration. A comparison with previously reported conditions for the same reaction, using organic solvents or solvent-free conditions, demonstrated the advantages of the "on-water" methodology, namely shorter reaction times, higher yields, simple workup, milder reaction conditions and the absence of a catalyst. supersaturated water-based solvent obtained by supersaturation of water (~18% w/w) with carbohydrates, an organic acid and an organic ketone [96]. The second-order rate constant (k2, 7.92 × 10 −5 M −1 s −1 ) determined for the reaction carried at room temperature is about 26-fold higher than that obtained for the same reaction in water. This rate enhancement was attributed to the combined presence of OH groups from the carbohydrates, which allows multiple hydrogen bonding sites, and the hydrophobic effect by water molecules. It is noteworthy that it is also possible to carry out the reaction of cyclopentadiene (39) and methyl acrylate (51a) using eutectic mixtures of carbohydrates as solvent medium; however, to ensure these mixtures were in a liquid state, higher temperatures (>85 °C) were required (cf. Scheme 11) [66,96].

Noncatalyzed Diels-Alder Cycloaddition Reactions
Romám and coworkers reported a catalyst-free protocol for the Diels-Alder cycloaddition of water-insoluble furan derivatives and N-substituted maleimides using "on-water" conditions [97]. The reaction of furans 102 and maleimides 55 carried out at room temperature afforded cycloadducts 103 and 104 in quantitative yields and endoselectivity (Scheme 25a). When the reaction was carried out at 65 °C, the reaction times were shortened and an increase in the exo-adducts was observed. On the other hand, the reaction between furfural N,N-dimethylhydrazone (105) and maleimides 55 afforded selectively the exo-adducts 106 obtained as single products, mixtures of 106 and phthalimides 107, or 107 as the sole products, depending on the maleimide precursors and reaction conditions (Scheme 25b). Upon heating, cycloadducts 106 can be converted into the corresponding phthalimides 107, whose formation was rationalized considering the ring-opening of the exo-7-oxabicycle followed by dehydration. A comparison with previously reported conditions for the same reaction, using organic solvents or solventfree conditions, demonstrated the advantages of the "on-water" methodology, namely shorter reaction times, higher yields, simple workup, milder reaction conditions and the absence of a catalyst. The aqueous Diels-Alder cycloaddition reaction of bio-based furans derived from renewable feedstocks represents a valuable example of a green and sustainable process in organic synthesis. Hailes and coworkers reported the synthesis of phthalimide-hydrazones 110 via an uncatalyzed one-pot tandem reaction in water starting from substituted furfurals 108 (Scheme 26a) [98]. The three-step cascade protocol involves the initial in situ formation of hydrazones 109 by reacting 108 and N,N-dimethylhydrazine, cycloaddition reaction with maleimides 55 and subsequent aromatization. The cycloaddition/aromatization also works for the reaction of hydrazone 109a with non-maleimide dienophiles 111, acrylonitrile and fumaronitrile, affording benzonitrile-hydrazones 112 in moderate yields (24-68%) (Scheme 26b). The one-pot three-step reaction of furfural 108a (R 1 = R 2 = R 3 = H) in the presence of dimethyl maleate afforded the corresponding cycloadduct, albeit in low yield. initial in situ formation of hydrazones 109 by reacting 108 and N,N-dimethylhydrazine, cycloaddition reaction with maleimides 55 and subsequent aromatization. The cycloaddition/aromatization also works for the reaction of hydrazone 109a with nonmaleimide dienophiles 111, acrylonitrile and fumaronitrile, affording benzonitrilehydrazones 112 in moderate yields (24-68%) (Scheme 26b). The one-pot three-step reaction of furfural 108a (R 1 = R 2 = R 3 = H) in the presence of dimethyl maleate afforded the corresponding cycloadduct, albeit in low yield. Ananikov and coworkers disclosed a three-step synthesis of polycyclic compound 116 from bio-based 5-(hydroxymethyl)furfural (HMF) (113) involving a Diels-Alder cycloaddition step (Scheme 27) [99]. Computational calculations demonstrated that the Diels-Alder reaction of 2,5-bis(hydroxymethyl)furan (BHMF) (114) and maleimide is energetically more favorable than that of HMF (113) with the same dienophile. Thus, HMF (113) was reduced to BHMF (114) in aqueous solution. Subsequent cycloaddition reaction of 114 with maleimide (55d) in water furnished compound 115 diastereoselectively (96% de) as the endo-adduct in 67% yield. To prevent the retro-Diels-Alder transformation, 115 was further reduced, giving compound 116 in 87% yield (58% overall yield). It is noteworthy that the three-step one-pot protocol in water, starting from HMF (113), proved to be more efficient, allowing the synthesis of 116 in 73% yield. Ananikov and coworkers disclosed a three-step synthesis of polycyclic compound 116 from bio-based 5-(hydroxymethyl)furfural (HMF) (113) involving a Diels-Alder cycloaddition step (Scheme 27) [99]. Computational calculations demonstrated that the Diels-Alder reaction of 2,5-bis(hydroxymethyl)furan (BHMF) (114) and maleimide is energetically more favorable than that of HMF (113) with the same dienophile. Thus, HMF (113) was reduced to BHMF (114) in aqueous solution. Subsequent cycloaddition reaction of 114 with maleimide (55d) in water furnished compound 115 diastereoselectively (96% de) as the endo-adduct in 67% yield. To prevent the retro-Diels-Alder transformation, 115 was further reduced, giving compound 116 in 87% yield (58% overall yield). It is noteworthy that the three-step one-pot protocol in water, starting from HMF (113), proved to be more efficient, allowing the synthesis of 116 in 73% yield.
cycloaddition reaction with maleimides 55 and subsequent aromatization. The cycloaddition/aromatization also works for the reaction of hydrazone 109a with nonmaleimide dienophiles 111, acrylonitrile and fumaronitrile, affording benzonitrilehydrazones 112 in moderate yields (24-68%) (Scheme 26b). The one-pot three-step reaction of furfural 108a (R 1 = R 2 = R 3 = H) in the presence of dimethyl maleate afforded the corresponding cycloadduct, albeit in low yield. Ananikov and coworkers disclosed a three-step synthesis of polycyclic compound 116 from bio-based 5-(hydroxymethyl)furfural (HMF) (113) involving a Diels-Alder cycloaddition step (Scheme 27) [99]. Computational calculations demonstrated that the Diels-Alder reaction of 2,5-bis(hydroxymethyl)furan (BHMF) (114) and maleimide is energetically more favorable than that of HMF (113) with the same dienophile. Thus, HMF (113) was reduced to BHMF (114) in aqueous solution. Subsequent cycloaddition reaction of 114 with maleimide (55d) in water furnished compound 115 diastereoselectively (96% de) as the endo-adduct in 67% yield. To prevent the retro-Diels-Alder transformation, 115 was further reduced, giving compound 116 in 87% yield (58% overall yield). It is noteworthy that the three-step one-pot protocol in water, starting from HMF (113), proved to be more efficient, allowing the synthesis of 116 in 73% yield. Recently, the Bruijnincx group disclosed the Diels-Alder reaction of furfurals with water-soluble maleimides in aqueous medium [100]. The reaction of furfurals 117 with maleimides 55 at 60 • C in water furnished cycloadducts 118 and 119 in low to moderate yields (1-58%) with exo-selectivity (Scheme 28a). Different selectivity was observed for the Diels-Alder reaction of HMF (113) with a maleimide, which led to the formation of the endo-cycloadduct as the major product. It is noteworthy that for more lipophilic adducts (R 2 = H), an increased preference for dehydration of the geminal diol 118/119 back to the aldehydes 120/121 and partitioning to the organic phase was observed. DFT calculations demonstrated that the limitation of the Diels-Alder reaction of furfural, and other related electron-poor furans, is of thermodynamic rather than kinetic nature and can be circumvented by using water, which acts both as solvent and as reactant in the geminal diol formation. Hydration of the formyl group is thermodynamically possible whether it occurs prior to or after the cyclization step, by favoring the rate of the direct reaction or decreasing the rate of the retro-Diels-Alder reaction, respectively. aldehydes 120/121 and partitioning to the organic phase was observed. DFT calculations demonstrated that the limitation of the Diels-Alder reaction of furfural, and other related electron-poor furans, is of thermodynamic rather than kinetic nature and can be circumvented by using water, which acts both as solvent and as reactant in the geminal diol formation. Hydration of the formyl group is thermodynamically possible whether it occurs prior to or after the cyclization step, by favoring the rate of the direct reaction or decreasing the rate of the retro-Diels-Alder reaction, respectively. The same group reported the use of oxidized furfurals, furoic acids, as dienes in the aqueous Diels-Alder cycloaddition reaction with maleimides [101]. The base-mediated reaction of furoic acids 122 and maleimides 55, carried out in water under mild conditions, led to the formation of cycloadducts 123/124 in moderate to good yields and exo-selectivity (Scheme 28b). In this case, the cycloaddition reaction benefits from the rate enhancement caused by the water effect as well as from the activation of the 2-furoic acids by conversion to the corresponding carboxylate salts. Notably, the reaction also works well when using 2-furoic acid esters or furamides as dienes, affording selectively exo-adducts as major products in moderate to good yields. It is noteworthy that when 2-furoic acid esters are used as dienes, the system is no longer homogeneous and reactions proceed "on-water".
Ohmic heating (ΩH)-assisted synthesis has emerged as a new methodology in organic synthesis, circumventing some of the limitations presented by the microwave irradiation (MW) and conventional heating methods. The advantages of ΩH-assisted synthesis were illustrated by the Diels-Alder cycloaddition of 9hydroxymethylanthracene 54 with N-methylmaleimide (55b) under three different heating processes: conventional, MW and ohmic heating (Scheme 29a) [102]. After only two minutes of reaction, cycloadduct 125 was obtained in 80% yield using ohmic heating, whereas under microwave irradiation the yield was significantly lower (53%). The conventional heating conditions also afforded the desired product in relatively lower yield (57%).  The same group reported the use of oxidized furfurals, furoic acids, as dienes in the aqueous Diels-Alder cycloaddition reaction with maleimides [101]. The base-mediated reaction of furoic acids 122 and maleimides 55, carried out in water under mild conditions, led to the formation of cycloadducts 123/124 in moderate to good yields and exo-selectivity (Scheme 28b). In this case, the cycloaddition reaction benefits from the rate enhancement caused by the water effect as well as from the activation of the 2-furoic acids by conversion to the corresponding carboxylate salts. Notably, the reaction also works well when using 2-furoic acid esters or furamides as dienes, affording selectively exo-adducts as major products in moderate to good yields. It is noteworthy that when 2-furoic acid esters are used as dienes, the system is no longer homogeneous and reactions proceed "on-water".
Ohmic heating (ΩH)-assisted synthesis has emerged as a new methodology in organic synthesis, circumventing some of the limitations presented by the microwave irradiation (MW) and conventional heating methods. The advantages of ΩH-assisted synthesis were illustrated by the Diels-Alder cycloaddition of 9-hydroxymethylanthracene 54 with Nmethylmaleimide (55b) under three different heating processes: conventional, MW and ohmic heating (Scheme 29a) [102]. After only two minutes of reaction, cycloadduct 125 was obtained in 80% yield using ohmic heating, whereas under microwave irradiation the yield was significantly lower (53%). The conventional heating conditions also afforded the desired product in relatively lower yield (57%).
Ohmic heating was also successfully applied in the regioselective and site-selective synthesis of coumarinyl porphyrin derivatives (Scheme 29b) [103]. The sequential Knoevenagel condensation of 4-hydroxycoumarin 126 and aromatic aldehydes 127 leading to α-methylenechromane derivatives 128, followed by hetero-Diels-Alder reaction of these in situ generated dienes with 2-vinyl-5,10,15,20-tetraphenylporphyrinatozinc(II) (129), was performed in aqueous medium using ohmic and conventional heating. The ΩH-assisted synthesis provided the coumarinyl porphyrin derivatives 130 in higher yield and shorter reaction time. The higher efficiency of these transformations under ohmic heating was rationalized as resulting from the high heating rates achieved in the beginning of the reactions which may lead to a more uniform heating and to less decomposition of the reactants. Additionally, the electrical dynamic perturbation in ohmic heating may also influence the polarization of the reaction medium and improve the transport properties. Ohmic heating was also successfully applied in the regioselective and site-selective synthesis of coumarinyl porphyrin derivatives (Scheme 29b) [103]. The sequential Knoevenagel condensation of 4-hydroxycoumarin 126 and aromatic aldehydes 127 leading to α-methylenechromane derivatives 128, followed by hetero-Diels-Alder reaction of these in situ generated dienes with 2-vinyl-5,10,15,20tetraphenylporphyrinatozinc(II) (129), was performed in aqueous medium using ohmic and conventional heating. The ΩH-assisted synthesis provided the coumarinyl porphyrin derivatives 130 in higher yield and shorter reaction time. The higher efficiency of these transformations under ohmic heating was rationalized as resulting from the high heating rates achieved in the beginning of the reactions which may lead to a more uniform heating and to less decomposition of the reactants. Additionally, the electrical dynamic perturbation in ohmic heating may also influence the polarization of the reaction medium and improve the transport properties.
A series of diversely substituted 6H-benzo[c]chromenes 134 have been prepared via intramolecular Diels-Alder reactions of furan with unactivated alkenes in an aqueous medium under MW irradiation (Scheme 30) [104]. The reaction pathway involves the initial formation of cycloadduct 132 which undergoes ring-opening to give intermediate 133, followed by aromatization to yield the desired 6H-benzo[c]chromenes 134 in yields ranging from 45 to 85%. This methodology was successfully extended to the synthesis of 6H-benzo[c]chromen-8-ols by employing 2-(2-(propargyloxy)phenyl)furan derivatives as reactants; however, the use of a mixture H2O/EtOH (4:1) as reaction medium was required to attain good efficiency. The use of a thin film microfluidic platform, namely a vortex fluidic device (VFD promote Diels-Alder reactions between 9-substituted anthracenes 135 and N-substit maleimides 55 in media with a high mole fraction of water, without the need for catal has been disclosed by Raston and coworkers (Scheme 31) [105]. Using the confined m of VFD processing, a dynamic thin fluid film is formed on the walls of the tube w there is intensive shear, with high mass and heat transfer, thus accelerating the D Alder reaction by providing a constant "soft energy". Carrying out the reactions u the optimized VDF processing parameters (e.g., 5000 rpm, tilt angle θ = 45°), at 50 ° 10% ethanol in water, led to the formation of the expected cycloadducts 136 in goo excellent yield, after 30 min of reaction. In contrast to previous studies, in which a hi speed favored the reaction progress, it was observed that changing the speed had effect on the reaction outcome. In fact, for rotations higher than 5000 rpm, a slight decr in the yield was observed. The use of a thin film microfluidic platform, namely a vortex fluidic device (VFD), to promote Diels-Alder reactions between 9-substituted anthracenes 135 and N-substituted maleimides 55 in media with a high mole fraction of water, without the need for catalysts, has been disclosed by Raston and coworkers (Scheme 31) [105]. Using the confined mode of VFD processing, a dynamic thin fluid film is formed on the walls of the tube where there is intensive shear, with high mass and heat transfer, thus accelerating the Diels-Alder reaction by providing a constant "soft energy". Carrying out the reactions under the optimized VDF processing parameters (e.g., 5000 rpm, tilt angle θ = 45 • ), at 50 • C in 10% ethanol in water, led to the formation of the expected cycloadducts 136 in good to excellent yield, after 30 min of reaction. In contrast to previous studies, in which a higher speed favored the reaction progress, it was observed that changing the speed had little effect on the reaction outcome. In fact, for rotations higher than 5000 rpm, a slight decrease in the yield was observed.
has been disclosed by Raston and coworkers (Scheme 31) [105]. Using the confined mode of VFD processing, a dynamic thin fluid film is formed on the walls of the tube where there is intensive shear, with high mass and heat transfer, thus accelerating the Diels-Alder reaction by providing a constant "soft energy". Carrying out the reactions under the optimized VDF processing parameters (e.g., 5000 rpm, tilt angle θ = 45°), at 50 °C in 10% ethanol in water, led to the formation of the expected cycloadducts 136 in good to excellent yield, after 30 min of reaction. In contrast to previous studies, in which a higher speed favored the reaction progress, it was observed that changing the speed had little effect on the reaction outcome. In fact, for rotations higher than 5000 rpm, a slight decrease in the yield was observed. A synthetic methodology towards dipyrromethanes involving two consecutive Diels-Alder reactions of azoalkenes and pyrrole has been accomplished by Pinho e Melo and coworkers (Scheme 32) [106]. The base-mediated dehydrohalogenation of alkyl and aryl α,α-dihalohydrazones 69 originates azoalkenes 73 and 140 which undergo a hetero-Diels-Alder reaction with pyrrole to give selectively the desired dipyrromethanes 138 in moderate to good yields. The "on-water" reaction conditions afforded the target products in higher yields with significantly shorter reaction times and simpler purification procedures than carrying out the reaction in dichloromethane or in solvent-free conditions. This one-pot methodology was further applied to the synthesis of dipyrromethanes derived from α,α-dihalooximes and pyrrole. A synthetic methodology towards dipyrromethanes involving two consecutive Diels-Alder reactions of azoalkenes and pyrrole has been accomplished by Pinho e Melo and coworkers (Scheme 32) [106]. The base-mediated dehydrohalogenation of alkyl and aryl α,α-dihalohydrazones 69 originates azoalkenes 73 and 140 which undergo a hetero-Diels-Alder reaction with pyrrole to give selectively the desired dipyrromethanes 138 in moderate to good yields. The "on-water" reaction conditions afforded the target products in higher yields with significantly shorter reaction times and simpler purification procedures than carrying out the reaction in dichloromethane or in solvent-free conditions. This one-pot methodology was further applied to the synthesis of dipyrromethanes derived from α,αdihalooximes and pyrrole. The reactivity of phosphorylated nitrosoalkenes towards enol ethers and pyrrole has been explored by Palacios and coworkers (Scheme 33) [107,108]. The one-pot synthetic methodologies gave access to functionalized 4-phosphorylated 1,2-oxazines 144 and open-chain 2-substituted pyrroles 145 through the treatment of the α-halooxime precursors 141 with base, followed by [4 + 2] cycloaddition reaction of the in situ generated 142 with enol ethers and pyrrole, respectively, in a regioselective fashion. The formation of pyrroles 145 was rationalized considering the rearomatization of pyrrole unit of the firstly formed cycloadducts. The substrate scope includes nitrosoalkenes bearing a variety of substituents at C-3 (Me, Et, Ph and CO2Me) and C-4 (P(O)Ph2, P(O)(OEt)2). Once again, the "on-water" protocol showed higher chemical efficiency and selectivity than the solvent-free conditions or the use of organic solvents, leading to 1,2-oxazines 144 with excellent diastereoselectivity. The reactivity of phosphorylated nitrosoalkenes towards enol ethers and pyrrole has been explored by Palacios and coworkers (Scheme 33) [107,108]. The one-pot synthetic methodologies gave access to functionalized 4-phosphorylated 1,2-oxazines 144 and openchain 2-substituted pyrroles 145 through the treatment of the α-halooxime precursors 141 with base, followed by [4 + 2] cycloaddition reaction of the in situ generated 142 with enol ethers and pyrrole, respectively, in a regioselective fashion. The formation of pyrroles 145 was rationalized considering the rearomatization of pyrrole unit of the firstly formed cycloadducts. The substrate scope includes nitrosoalkenes bearing a variety of substituents at C-3 (Me, Et, Ph and CO 2 Me) and C-4 (P(O)Ph 2 , P(O)(OEt) 2 ). Once again, the "on-water" protocol showed higher chemical efficiency and selectivity than the solvent-free conditions or the use of organic solvents, leading to 1,2-oxazines 144 with excellent diastereoselectivity. 142 with enol ethers and pyrrole, respectively, in a regioselective fashion. The formation of pyrroles 145 was rationalized considering the rearomatization of pyrrole unit of the firstly formed cycloadducts. The substrate scope includes nitrosoalkenes bearing a variety of substituents at C-3 (Me, Et, Ph and CO2Me) and C-4 (P(O)Ph2, P(O)(OEt)2). Once again, the "on-water" protocol showed higher chemical efficiency and selectivity than the solvent-free conditions or the use of organic solvents, leading to 1,2-oxazines 144 with excellent diastereoselectivity.

Scheme 33. Hetero-Diels-Alder reaction of phosphinyl nitrosoalkenes with pyrrole and enol ethers in water.
A chemo-and diastereoselective synthetic multicomponent route to pyrazolotetrahydropyridines involving an intramolecular aza-Diels-Alder reaction was disclosed by Shaabani and coworkers (Scheme 34) [109]. A plethora of pyrazolotetrahydropyridines 151 was efficiently prepared from benzoylacetonitrile derivatives 146, hydrazines 147, aromatic aldehydes 150 and styrenesulfonyl or cinnamoyl chloride in water in the presence of base, using the group-assisted purification (GAP) chemistry strategy. In this one-pot procedure, 5-amino-pyrazoles 148 were initially formed from benzoylacetonitrile derivatives 146 and hydrazines 147 through tandem condensation and Scheme 33. Hetero-Diels-Alder reaction of phosphinyl nitrosoalkenes with pyrrole and enol ethers in water.
A chemo-and diastereoselective synthetic multicomponent route to pyrazolotetrahydropyridines involving an intramolecular aza-Diels-Alder reaction was disclosed by Shaabani and coworkers (Scheme 34) [109]. A plethora of pyrazolo-tetrahydropyridines 151 was efficiently prepared from benzoylacetonitrile derivatives 146, hydrazines 147, aromatic aldehydes 150 and styrenesulfonyl or cinnamoyl chloride in water in the presence of base, using the group-assisted purification (GAP) chemistry strategy. In this one-pot procedure, 5-amino-pyrazoles 148 were initially formed from benzoylacetonitrile derivatives 146 and hydrazines 147 through tandem condensation and thermal cyclization, under solvent-free conditions at 120 • C. Then, intermediates 148 reacted chemoselectively with 2-formylphenyl-(E)-2-phenylethenesulfonate derivatives (e.g., 154), generated in situ from 149 and 150, to give intermediate 155 which undergoes an intramolecular aza-Diels-Alder reaction via exo-approach to yield pyrazolo-tetrahydropyridines 151 as single diastereoisomers (Scheme 34). The proposed reaction mechanism was corroborated by some control experiments in which the synthesis of an intermediate (e.g., 155) was accomplished.
Vilches-Herrera and coworkers developed a microwave-assisted methodology for the preparation of annulated tetrahydropyridines by intramolecular aza-Diels-Alder reaction (Scheme 35) [110]. Featuring several requirements for sustainable chemistry such as the use of water as solvent, microwave irradiation, absence of catalyst and easy product isolation by precipitation, it gives access to important scaffolds bearing the tetrahydropyridine and the chromane moieties. Under the optimized reaction conditions at 200 • C, a range of alkenyl 2-iminopyrroles and 2-iminopyrazoles 156 underwent intramolecular aza-Diels-Alder reaction giving rise to the corresponding dihydrochromeno-pyrrolo-and dihydrochromenopyrazolo-tetrahydropyridines 157 in moderate to high yield and with overall excellent transdiastereoselectivity. Moreover, when propargylic derivatives were used as dienophiles, aromatic annulated pyridines 158 were isolated in good yields. As observed for other aza-Diels-Alder reactions, the stereoselectivity of the process was strongly dependent on the solvent used, with selective formation of trans-157 when reactions were performed in water, whereas the use of nonpolar solvents such p-xylene led to a mixture of cis/trans-157 products. thermal cyclization, under solvent-free conditions at 120 °C. Then, intermediates 148 reacted chemoselectively with 2-formylphenyl-(E)-2-phenylethenesulfonate derivatives (e.g., 154), generated in situ from 149 and 150, to give intermediate 155 which undergoes an intramolecular aza-Diels-Alder reaction via exo-approach to yield pyrazolotetrahydropyridines 151 as single diastereoisomers (Scheme 34). The proposed reaction mechanism was corroborated by some control experiments in which the synthesis of an intermediate (e.g., 155) was accomplished.

Scheme 34. Multicomponent synthesis of pyrazolo-tetrahydropyridines via intramolecular aza-Diels-Alder reaction in water.
Vilches-Herrera and coworkers developed a microwave-assisted methodology for the preparation of annulated tetrahydropyridines by intramolecular aza-Diels-Alder reaction (Scheme 35) [110]. Featuring several requirements for sustainable chemistry such as the use of water as solvent, microwave irradiation, absence of catalyst and easy product isolation by precipitation, it gives access to important scaffolds bearing the tetrahydropyridine and the chromane moieties. Under the optimized reaction conditions at 200 °C, a range of alkenyl 2-iminopyrroles and 2-iminopyrazoles 156 underwent intramolecular aza-Diels-Alder reaction giving rise to the corresponding dihydrochromeno-pyrrolo-and dihydrochromeno-pyrazolo-tetrahydropyridines 157 in moderate to high yield and with overall excellent trans-diastereoselectivity. Moreover, when propargylic derivatives were used as dienophiles, aromatic annulated pyridines 158 were isolated in good yields. As observed for other aza-Diels-Alder reactions, the stereoselectivity of the process was strongly dependent on the solvent used, with selective formation of trans-157 when reactions were performed in water, whereas the use of nonpolar solvents such p-xylene led to a mixture of cis/trans-157 products. A multicomponent chemo-, regio-and stereoselective approach to spiro{pyrazolo[1.3]-dioxanopyridine}-4,6-diones and spiro{isoxazolo[1.3]-dioxanopyridine}-4,6-diones derivatives 161 carried out in water under microwave irradiation was reported by Tu and Li (Scheme 36a) [111]. Using Meldrum's acid (159), a wide variety of aromatic aldehydes and 3-methylisoxazol-5-amine (160a) or 3-methyl-1phenylpyrazol-5-amine (160b) as substrates, the target products 161 were obtained in high yield within a very short reaction time (9-13 min). The key step in this domino reaction involves the hetero-Diels-Alder reaction between imine 162 and Knoevenagel adduct 163, which follows the endo rule and gives rise to syn-161 as single stereoisomers. Interestingly, a different chemoselectivity was observed when N-H-and N-Me-pyrazol-5-amines were employed, leading to pyrazolo [3,4-b]pyridines in high yields. This outcome resulted from a different reaction pathway in which a Michael addition of pyrazole's amino group onto intermediate 166 occurs, followed by addition to the carbonyl favored by the higher reactivity of the amino group. This protocol was further applied to the synthesis of pyrimidinespiroisoxazolo [5,4-b]pyridines 165 (Scheme 36b) [112]. Under the same reaction conditions, barbituric acids 164, two equivalents of aromatic aldehydes and 3methylisoxazol-5-amine (160a) provided the desired syn-165 in yields ranging from 78 to 89%.

Scheme 35. Stereoselective synthesis of annulated tetrahydropyridines via intramolecular aza-Diels-Alder reaction in water.
A multicomponent chemo-, regio-and stereoselective approach to spiro{pyrazolo[1.3]-dioxanopyridine}-4,6-diones and spiro{isoxazolo[1.3]-dioxanopyridine}-4,6-diones derivatives 161 carried out in water under microwave irradiation was reported by Tu and Li (Scheme 36a) [111]. Using Meldrum's acid (159), a wide variety of aromatic aldehydes and 3-methylisoxazol-5-amine (160a) or 3-methyl-1-phenylpyrazol-5-amine (160b) as substrates, the target products 161 were obtained in high yield within a very short reaction time (9-13 min). The key step in this domino reaction involves the hetero-Diels-Alder reaction between imine 162 and Knoevenagel adduct 163, which follows the endo rule and gives rise to syn-161 as single stereoisomers. Interestingly, a different chemoselectivity was observed when N-H-and N-Me-pyrazol-5-amines were employed, leading to pyrazolo [3,4-b]pyridines in high yields. This outcome resulted from a different reaction pathway in which a Michael addition of pyrazole's amino group onto intermediate 166 occurs, followed by addition to the carbonyl favored by the higher reactivity of the amino group. This protocol was further applied to the synthesis of pyrimidinespiroisoxazolo [5,4b]pyridines 165 (Scheme 36b) [112]. Under the same reaction conditions, barbituric acids 164, two equivalents of aromatic aldehydes and 3-methylisoxazol-5-amine (160a) provided the desired syn-165 in yields ranging from 78 to 89%. which follows the endo rule and gives rise to syn-161 as single stereoisomers. Interestingly, a different chemoselectivity was observed when N-H-and N-Me-pyrazol-5-amines were employed, leading to pyrazolo [3,4-b]pyridines in high yields. This outcome resulted from a different reaction pathway in which a Michael addition of pyrazole's amino group onto intermediate 166 occurs, followed by addition to the carbonyl favored by the higher reactivity of the amino group. This protocol was further applied to the synthesis of pyrimidinespiroisoxazolo [5,4-b]pyridines 165 (Scheme 36b) [112]. Under the same reaction conditions, barbituric acids 164, two equivalents of aromatic aldehydes and 3methylisoxazol-5-amine (160a) provided the desired syn-165 in yields ranging from 78 to 89%.  [113,114]. The mechanism involves initial Knoevenagel condensation to give the heterodiene intermediates 172 or 173, followed by an intramolecular aza-Diels-Alder reaction to afford the corresponding heteropolycyclic compounds in high yield. The high efficiency of these catalyst-free transformations, as well as the observed regioselectivity in the synthesis of 171, was attributed to the presence of the softer sulfur atom in the diene moiety. This reactivity was further extended to O-allylsalicylaldehydes which under the same reaction conditions originated cis-annulated [6,6]-fused thiopyrano benzopyran derivatives in a highly regioand stereoselective fashion [115].
Moghaddam and coworkers demonstrated that O-acrylated salicylaldehydes 174 can also undergo DKHDA with dihydroindole-2-thiones (e.g., 168a) in water under reflux to afford polycyclic indole-annulated thiopyranocoumarin derivatives, in good to high yields with high regio-and stereoselectivity [116]. However, a different outcome was observed in the DKHDA of these dienophiles 174 with 4-hydroxydithiocoumarin 170 (Scheme 38) [117]. Although the efficiency of the domino reaction remained high, yielding thiochromoneannulated thiopyranocoumarin 175 and 176 in good overall yield, the diastereoselectivity of the domino reaction varied significantly with the substituents on the O-acrylated salicylaldehydes, namely the substituent on the carbon-carbon double bond (R 3 ). Thus, methyl-substituted O-acrylated salicylaldehydes 174 afforded selectively cis-176 via an endo-transition state, whereas phenyl-substituted O-acrylated salicylaldehydes 174 gave predominantly trans-175 resulting from an exo-transition state. the heterodiene intermediates 172 or 173, followed by an intramolecular aza-Diels-Alder reaction to afford the corresponding heteropolycyclic compounds in high yield. The high efficiency of these catalyst-free transformations, as well as the observed regioselectivity in the synthesis of 171, was attributed to the presence of the softer sulfur atom in the diene moiety. This reactivity was further extended to O-allylsalicylaldehydes which under the same reaction conditions originated cis-annulated [6,6]-fused thiopyrano benzopyran derivatives in a highly regio-and stereoselective fashion [115]. Scheme 37. Domino Knoevenagel/hetero-Diels-Alder reaction in water as an approach to polycyclic heterocycles.
Initial Knoevenagel reaction of aldehydes 177 with dimedone 149, N,Ndimethylbarbituric acid (164a) or indoline-2-thiones 168 generates the dienophile tethered to the corresponding diene moiety by a sulfonate link, which undergoes intramolecular hetero-Diels-Alder reaction to give the desired annulated benzo-δ-sultone derivatives in moderate to high yield, with good to high diastereoselectivity. As in the aforementioned methodologies, the reactions were carried out in refluxing water under catalyst-free conditions, affording the cis-trans-annulated cycloadducts as major isomers.
The one-pot three-component synthesis of a range of pentacyclic-fused pyranochromenone and pyranoquinolinone benzosultone derivatives was successfully accomplished by Ghandi and coworkers (Scheme 42) [122]. The developed synthetic methodology involved successive addition of 2-hydroxybenzaldehydes 187, 4-hydroxycoumarins 185 and a catalytic amount of EDDA to an aqueous solution of styrenesulfonyl chloride and K 2 CO 3 , followed by refluxing conditions. The reactions proceeded smoothly through O-sulfonylation/ Knoevenagel condensation/hetero-Diels-Alder reaction cascade affording cis-trans-annulated coumarins 188 as major products in good to high yields. Similarly, when 4-hydroxy-2quinolones were used, cis-trans-pyranoquinolinone benzosultone derivatives were obtained selectively, thus demonstrating that the hetero-Diels-Alder reaction proceeds via endo-E-syn transition states. A range of pyrano[2,3-d]pyrimidines were efficiently prepared through a threecomponent one-pot domino Knoevenagel/Diels-Alder reaction in aqueous suspension (Scheme 43) [123]. Reactions of barbituric acids, aldehydes and ethyl vinyl ether were performed at room temperature, while the use of a styrene derivative or N-vinyl-2oxazolidinone as dienophiles required increasing the reaction temperature to 60 °C. These transformations were highly diastereoselective, furnishing preferentially or exclusively the endo-cis-annulated uracils 191 and 192 in high yields. Along with pyrano[2,3d]pyrimidines 192, 5-methyl-substituted derivatives 193 arising from the reaction with in situ generated acetaldehyde were also formed as minor products. A range of pyrano [2,3-d]pyrimidines were efficiently prepared through a threecomponent one-pot domino Knoevenagel/Diels-Alder reaction in aqueous suspension (Scheme 43) [123]. Reactions of barbituric acids, aldehydes and ethyl vinyl ether were performed at room temperature, while the use of a styrene derivative or N-vinyl-2-oxazolidinone as dienophiles required increasing the reaction temperature to 60 • C. These transformations were highly diastereoselective, furnishing preferentially or exclusively the endo-cisannulated uracils 191 and 192 in high yields. Along with pyrano[2,3-d]pyrimidines 192, 5-methyl-substituted derivatives 193 arising from the reaction with in situ generated acetaldehyde were also formed as minor products.
(Scheme 43) [123]. Reactions of barbituric acids, aldehydes and ethyl vinyl ether were performed at room temperature, while the use of a styrene derivative or N-vinyl-2oxazolidinone as dienophiles required increasing the reaction temperature to 60 °C. These transformations were highly diastereoselective, furnishing preferentially or exclusively the endo-cis-annulated uracils 191 and 192 in high yields. Along with pyrano [2,3d]pyrimidines 192, 5-methyl-substituted derivatives 193 arising from the reaction with in situ generated acetaldehyde were also formed as minor products.  [124]. It was experimentally observed that the multicomponent reaction performed in water leads to dehydropyran 197 in higher yield than that carried out in water-miscible organic solvents (e.g., THF, acetonitrile) or water-immiscible solvents (e.g., CHCl3 or toluene). On the other hand, the mechanistic studies revealed the role of water in the elimination step leading to 199, which favors the formation of six-membered transition state 198 and consequently a lower activation free energy barrier. In addition, it was found that owing to the presence of water, the activation free energy barriers of all chemical steps involved in the Knoevenagel/hetero-Diels-Alder sequence were lower than 39 kcal mol −1 at 25 °C, thus confirming that the use of catalyst is not necessary for the reaction to occur. Frapper et al. investigated experimentally and theoretically the role of water in a Knoevenagel/hetero-Diels-Alder sequence involving α-methylstyrene 194, formaldehyde (195) and 2,4-pentanedione (196) as reactants (Scheme 44) [124]. It was experimentally observed that the multicomponent reaction performed in water leads to dehydropyran 197 in higher yield than that carried out in water-miscible organic solvents (e.g., THF, acetonitrile) or water-immiscible solvents (e.g., CHCl 3 or toluene). On the other hand, the mechanistic studies revealed the role of water in the elimination step leading to 199, which favors the formation of six-membered transition state 198 and consequently a lower activation free energy barrier. In addition, it was found that owing to the presence of water, the activation free energy barriers of all chemical steps involved in the Knoevenagel/hetero-Diels-Alder sequence were lower than 39 kcal mol −1 at 25 • C, thus confirming that the use of catalyst is not necessary for the reaction to occur. The furan/maleimide Diels-Alder reaction has been used for the covalent functionalization of graphene with polymers; however, in general, long reaction times and high temperatures were required. Recently, Lim and coworkers reported a mild protocol for the covalent direct functionalization of reduced graphene oxide (rGO) by furan/maleimide Diels-Alder click reaction in water [125]. rGO/PSMF hybrids 201 were obtained by reaction of rGO with poly(styrene-alt-maleic anhydride) bearing furfuryl groups (PSMF) 200 under ultrasound irradiation at a frequency of 35 kHz (Scheme 45). It is noteworthy that under these conditions, rGO/PSMF hybrids 201 were obtained with 13 wt% grafted PSMF, while for the reaction under conventional stirring conditions over 48 h, the grafting was only 8 wt%, thus demonstrating the ability of sonication to accelerate the Diels-Alder reaction. The furan/maleimide Diels-Alder reaction has been used for the covalent functionalization of graphene with polymers; however, in general, long reaction times and high temperatures were required. Recently, Lim and coworkers reported a mild protocol for the covalent direct functionalization of reduced graphene oxide (rGO) by furan/maleimide Diels-Alder click reaction in water [125]. rGO/PSMF hybrids 201 were obtained by reaction of rGO with poly(styrene-alt-maleic anhydride) bearing furfuryl groups (PSMF) 200 under ultrasound irradiation at a frequency of 35 kHz (Scheme 45). It is noteworthy that under these conditions, rGO/PSMF hybrids 201 were obtained with 13 wt% grafted PSMF, while for the reaction under conventional stirring conditions over 48 h, the grafting was only 8 wt%, thus demonstrating the ability of sonication to accelerate the Diels-Alder reaction.

196
In the last decade, the furan/maleimide Diels-Alder click reaction in water has found wide application in the synthesis of biopolymer-based hydrogels. Wei and coworkers reported the synthesis of thermoresponsive hydrogels 204 through a Diels-Alder reaction in water between poly(N,N-dimethylacrylamide-co-furfuryl methacrylate) 202 and N-maleolyl alanine poly(ethylene glycol) 203 (Scheme 46) [126]. The reaction proceeds efficiently under mild conditions (37 • C) in the absence of catalysts, initiators or coupling reagents, thus providing an alternative to conventional conjugation strategies such as copper-catalyzed azide-alkyne cycloaddition whose intrinsic toxicity limits its application in biological systems. It is noteworthy that the hydrogels 204 are stable in water and that the thermal reversibility was demonstrated since the retro-Diels-Alder reaction could be carried out easily in N,N-dimethylformamide at higher temperatures (80-100 • C). The aqueous Diels-Alder click reaction was also applied to the synthesis of degradable poly(ethylene glycol)based hydrogels using maleimide-and furyl-substituted PEG macromonomers as starting materials [127]. In this case, hydrogel degradation occurs within days to weeks at body temperature via retro-Diels-Alder reaction followed by hydrolysis of the maleimide groups. The straightforwardness of the synthesis and the degradability of these hydrogels make them valuable biomaterials for application in controlled drug/protein release or in the area of tissue engineering, where degradation of the biomaterial is often necessary. Scheme 44. Multicomponent reaction in water towards dihydropyrans.
The furan/maleimide Diels-Alder reaction has been used for the covalent functionalization of graphene with polymers; however, in general, long reaction times and high temperatures were required. Recently, Lim and coworkers reported a mild protocol for the covalent direct functionalization of reduced graphene oxide (rGO) by furan/maleimide Diels-Alder click reaction in water [125]. rGO/PSMF hybrids 201 were obtained by reaction of rGO with poly(styrene-alt-maleic anhydride) bearing furfuryl groups (PSMF) 200 under ultrasound irradiation at a frequency of 35 kHz (Scheme 45). It is noteworthy that under these conditions, rGO/PSMF hybrids 201 were obtained with 13 wt% grafted PSMF, while for the reaction under conventional stirring conditions over 48 h, the grafting was only 8 wt%, thus demonstrating the ability of sonication to accelerate the Diels-Alder reaction. Scheme 45. Ultrasound-accelerated covalent functionalization of rGO with poly(styrene-alt-maleic anhydride) by Diels-Alder click reaction in water.
In the last decade, the furan/maleimide Diels-Alder click reaction in water has found wide application in the synthesis of biopolymer-based hydrogels. Wei and coworkers reported the synthesis of thermoresponsive hydrogels 204 through a Diels-Alder reaction in water between poly(N,N-dimethylacrylamide-co-furfuryl methacrylate) 202 and Nmaleolyl alanine poly(ethylene glycol) 203 (Scheme 46) [126]. The reaction proceeds efficiently under mild conditions (37 °C) in the absence of catalysts, initiators or coupling reagents, thus providing an alternative to conventional conjugation strategies such as copper-catalyzed azide-alkyne cycloaddition whose intrinsic toxicity limits its application in biological systems. It is noteworthy that the hydrogels 204 are stable in water and that the thermal reversibility was demonstrated since the retro-Diels-Alder reaction could be carried out easily in N,N-dimethylformamide at higher temperatures (80-100 °C). The aqueous Diels-Alder click reaction was also applied to the synthesis of degradable poly(ethylene glycol)-based hydrogels using maleimide-and furylsubstituted PEG macromonomers as starting materials [127]. In this case, hydrogel degradation occurs within days to weeks at body temperature via retro-Diels-Alder In 2011, Shoichet and coworkers disclosed the first synthesis of cross-linked hyaluronic acid (HA) hydrogels based on Diels-Alder click chemistry [128]. The synthetic procedure, involving a clean one-step, catalyst-free, aqueous-based Diels-Alder reaction between furan-modified HA derivatives 205 and dimaleimide poly(ethylene glycol) 206, led to the formation of cytocompatible HA-PEG hydrogels 207 with potential application in tissue engineering and regenerative medicine (Scheme 47). In 2011, Shoichet and coworkers disclosed the first synthesis of cross-linked hyaluronic acid (HA) hydrogels based on Diels-Alder click chemistry [128]. The synthetic procedure, involving a clean one-step, catalyst-free, aqueous-based Diels-Alder reaction between furan-modified HA derivatives 205 and dimaleimide poly(ethylene glycol) 206, led to the formation of cytocompatible HA-PEG hydrogels 207 with potential application in tissue engineering and regenerative medicine (Scheme 47).
In 2011, Shoichet and coworkers disclosed the first synthesis of cross-linked hyaluronic acid (HA) hydrogels based on Diels-Alder click chemistry [128]. The synthetic procedure, involving a clean one-step, catalyst-free, aqueous-based Diels-Alder reaction between furan-modified HA derivatives 205 and dimaleimide poly(ethylene glycol) 206, led to the formation of cytocompatible HA-PEG hydrogels 207 with potential application in tissue engineering and regenerative medicine (Scheme 47). Scheme 47. Diels-Alder reaction of furan-modified HA derivatives and dimaleimide poly(ethylene glycol) in aqueous medium.
In the same year, Marra and coworkers reported the synthesis of polysaccharide biodegradable hydrogels 210 for protein encapsulation via the Diels-Alder reaction of maleimide-functionalized HA 208 and furan-functionalized HA 209 using water as solvent medium (Scheme 48) [129]. The cycloaddition reaction was selective and efficient for the polysaccharide bioconjugation, allowing the direct encapsulation of positive and negative proteins, lysosome and insulin, respectively, in the biodegradable hydrogels within 40 min of gelation time. Furthermore, it has been shown that proteins can be released from the hydrogel into the local microenvironment in a controlled manner. The Scheme 47. Diels-Alder reaction of furan-modified HA derivatives and dimaleimide poly(ethylene glycol) in aqueous medium.
In the same year, Marra and coworkers reported the synthesis of polysaccharide biodegradable hydrogels 210 for protein encapsulation via the Diels-Alder reaction of maleimide-functionalized HA 208 and furan-functionalized HA 209 using water as solvent medium (Scheme 48) [129]. The cycloaddition reaction was selective and efficient for the polysaccharide bioconjugation, allowing the direct encapsulation of positive and negative proteins, lysosome and insulin, respectively, in the biodegradable hydrogels within 40 min of gelation time. Furthermore, it has been shown that proteins can be released from the hydrogel into the local microenvironment in a controlled manner. The furanand maleimide-functionalized polysaccharide coupling via aqueous Diels-Alder reaction was also explored for the development of controlled drug delivery systems, namely the synthesis of biodegradable hyaluronic acid hydrogels to control the release of dexamethasone [130]. In this case, furan-and maleimide-functionalized hyaluronic acids were used to conjugate the hydrogel, and furan-functionalized dexamethasone was used for the covalent immobilization. furan-and maleimide-functionalized polysaccharide coupling via aqueous Diels-Alder reaction was also explored for the development of controlled drug delivery systems, namely the synthesis of biodegradable hyaluronic acid hydrogels to control the release of dexamethasone [130]. In this case, furan-and maleimide-functionalized hyaluronic acids were used to conjugate the hydrogel, and furan-functionalized dexamethasone was used for the covalent immobilization.
The aqueous furan/maleimide Diels-Alder click reaction strategy was also applied to the synthesis of thermally reversible nanocellulose hydrogels using furan-functionalized nanocellulose fibers and water-soluble oligoether bismaleimides [131]. In this case, the cross-linking reaction was carried out at 65 °C, and the reaction could be reverted at 95  The aqueous furan/maleimide Diels-Alder click reaction strategy was also applied to the synthesis of thermally reversible nanocellulose hydrogels using furan-functionalized nanocellulose fibers and water-soluble oligoether bismaleimides [131]. In this case, the cross-linking reaction was carried out at 65 • C, and the reaction could be reverted at 95 • C via retro-Diels-Alder reaction.
Recently, the synthesis of self-healing pectin/chitosan hybrid hydrogels for drug delivery via Diels-Alder coupling in aqueous medium has also been reported [132]. These polysaccharide biocompatible hydrogels were efficiently obtained through the Diels-Alder reaction of furan-functionalized pectin and maleimide-functionalized chitosan at 65 • C over 5 h, and they showed high swelling properties, pH-responsiveness and cytocompatibility.
Gabilondo's group reported the synthesis of several biocompatible hydrogels by the Diels-Alder click cross-linking reaction between functionalized furans and maleimides in water, namely methacrylate-based hydrogels [133], methacrylate/polyetheramine [134] and starch/graphene crosslinked hydrogels [135], chitosan-based hydrogels [136] and starch-based nanocomposite hydrogels [137]. The starch-based nanocomposite hydrogels were prepared through the Diels-Alder click reaction between a furan-functionalized starch derivative 211 and a water-soluble PEG-based tetramaleimide 212, followed by the addition of cellulose nanocrystals as nanoreinforcement (Scheme 49) [137]. The reaction, performed at 65 • C over 24 h, afforded hydrogels 213 as solid-like robust materials that keep the shape in their hydrated form. It is noteworthy that the incorporation of cellulose nanocrystals influences the morphology of the hydrogels and the drug delivery performance of the materials.

Catalyzed Diels-Alder Cycloaddition Reactions
The aforementioned MCPRs can be classified into ABC and ACC', referring to the classical conditions (aniline, aldehyde and nucleophilic alkenes) and the use of aniline and two equivalents of a nucleophilic alkene, respectively. One example of the latter, the synthesis of furano[3,2-c]-1,2,3,4-tetrahydroquinolines involving the MCPR between anilines 2 and two equivalents of 2,3-dihydrofuran (6), has been recently reported by Fernandes and coworkers (Scheme 50) [138]. Using water as solvent and p-sulfonic acid calix [4]arene (CX4SO3H) as organocatalyst, a series of tetrahydroquinoline derivatives 214 were prepared in moderate to excellent yield, with aniline and 4-halo-anilines providing the target products in the highest yields (85-95%). The catalyst CX4SO3H could be reused up to four times while maintaining the catalytic activity. Isotopic labeling experiments involving the synthesis of furano[3,2-c]-1,2,3,4-tetrahydroquinoline 216, supported by NMR and mass spectroscopy data, were crucial for the validation of the reaction Scheme 49. Starch-based nanocomposite hydrogel via Diels-Alder reaction of a furan-functionalized starch derivative and a water-soluble PEG-based tetramaleimide in aqueous medium.

Catalyzed Diels-Alder Cycloaddition Reactions
The aforementioned MCPRs can be classified into ABC and ACC', referring to the classical conditions (aniline, aldehyde and nucleophilic alkenes) and the use of aniline and two equivalents of a nucleophilic alkene, respectively. One example of the latter, the synthesis of furano[3,2-c]-1,2,3,4-tetrahydroquinolines involving the MCPR between anilines 2 and two equivalents of 2,3-dihydrofuran (6), has been recently reported by Fernandes and coworkers (Scheme 50) [138]. Using water as solvent and p-sulfonic acid calix [4]arene (CX4SO 3 H) as organocatalyst, a series of tetrahydroquinoline derivatives 214 were prepared in moderate to excellent yield, with aniline and 4-halo-anilines providing the target products in the highest yields (85-95%). The catalyst CX4SO 3 H could be reused up to four times while maintaining the catalytic activity. Isotopic labeling experiments involving the synthesis of furano[3,2-c]-1,2,3,4-tetrahydroquinoline 216, supported by NMR and mass spectroscopy data, were crucial for the validation of the reaction mechanism. The reaction seems to evolve through a stepwise sequence via ionic intermediates originating oxonium ion 215, which undergoes an intramolecular electrophilic aromatic substitution, under CX4SO 3 H catalysis, to afford the final products.
classical conditions (aniline, aldehyde and nucleophilic alkenes) and the use of aniline and two equivalents of a nucleophilic alkene, respectively. One example of the latter, the synthesis of furano[3,2-c]-1,2,3,4-tetrahydroquinolines involving the MCPR between anilines 2 and two equivalents of 2,3-dihydrofuran (6), has been recently reported by Fernandes and coworkers (Scheme 50) [138]. Using water as solvent and p-sulfonic acid calix [4]arene (CX4SO3H) as organocatalyst, a series of tetrahydroquinoline derivatives 214 were prepared in moderate to excellent yield, with aniline and 4-halo-anilines providing the target products in the highest yields (85-95%). The catalyst CX4SO3H could be reused up to four times while maintaining the catalytic activity. Isotopic labeling experiments involving the synthesis of furano[3,2-c]-1,2,3,4-tetrahydroquinoline 216, supported by NMR and mass spectroscopy data, were crucial for the validation of the reaction mechanism. The reaction seems to evolve through a stepwise sequence via ionic intermediates originating oxonium ion 215, which undergoes an intramolecular electrophilic aromatic substitution, under CX4SO3H catalysis, to afford the final products. The same group developed a highly efficient and green synthetic protocol for the preparation of julolidines based on the MCPRs approach, using the same catalyst (CX4SO 3 H) and star anise oil (93% content of trans-anethol) as dienophile (Scheme 51) [139]. A range of substituted anilines 2 reacted smoothly with formaldehyde (195) and trans-anethol (76), in water at 96 • C for 2.5 h, under CX4SO 3 H catalysis giving rise to the diastereoisomeric mixture of julolidines 217 and 218 in yields ranging from 15 to 85%. No significant diastereoisomer excess was observed, albeit the trans isomer was the major isomer in all cases. Although both electron-donating and -withdrawing groups were well tolerated, higher yields were attained with anilines bearing electron-withdrawing groups. Furthermore, the easy workup procedure allowed the organocatalyst to be reused up to four times without relevant loss of catalytic activity. The same group developed a highly efficient and green synthetic protocol for the preparation of julolidines based on the MCPRs approach, using the same catalyst (CX4SO3H) and star anise oil (93% content of trans-anethol) as dienophile (Scheme 51) [139]. A range of substituted anilines 2 reacted smoothly with formaldehyde (195) and trans-anethol (76), in water at 96 °C for 2.5 h, under CX4SO3H catalysis giving rise to the diastereoisomeric mixture of julolidines 217 and 218 in yields ranging from 15 to 85%. No significant diastereoisomer excess was observed, albeit the trans isomer was the major isomer in all cases. Although both electron-donating and -withdrawing groups were well tolerated, higher yields were attained with anilines bearing electron-withdrawing groups. Furthermore, the easy workup procedure allowed the organocatalyst to be reused up to four times without relevant loss of catalytic activity. The synthesis of julolidines through the one-pot cascade reaction of aniline derivatives 219 with a mixture of styrene (220) and formaldehyde (195) using silica sulfuric acid (SSA) as catalyst has also been reported (Scheme 52) [140]. Reactions were carried out in water under refluxing conditions for 24 h and led to the desired products 221 as diastereoisomeric mixtures in moderate to good yield. When o-substituted anilines were used, tetrahydroquinolines 222 were obtained, although the increase in reaction time (48 h)  The synthesis of julolidines through the one-pot cascade reaction of aniline derivatives 219 with a mixture of styrene (220) and formaldehyde (195) using silica sulfuric acid (SSA) as catalyst has also been reported (Scheme 52) [140]. Reactions were carried out in water under refluxing conditions for 24 h and led to the desired products 221 as diastereoisomeric mixtures in moderate to good yield. When o-substituted anilines were used, tetrahydroquinolines 222 were obtained, although the increase in reaction time (48 h) was required to attain good efficiency.
The synthesis of julolidines through the one-pot cascade reaction of aniline derivatives 219 with a mixture of styrene (220) and formaldehyde (195) using silica sulfuric acid (SSA) as catalyst has also been reported (Scheme 52) [140]. Reactions were carried out in water under refluxing conditions for 24 h and led to the desired products 221 as diastereoisomeric mixtures in moderate to good yield. When o-substituted anilines were used, tetrahydroquinolines 222 were obtained, although the increase in reaction time (48 h) was required to attain good efficiency. Scheme 52. One-pot tandem cascade three-component Povarov reaction towards julolidines in water.
Beifuss and coworkers developed a straightforward procedure for the diastereoselective synthesis of tetrahydroquinolines based on a domino process involving in situ reduction, imine formation and aza-Diels-Alder reaction (Scheme 53a) [141]. Using nitrobenzenes instead of the typical aniline derivatives, the domino process was triggered by in situ reduction of 224 with iron in combination with citric acid as chelating ligand and montmorillonite as catalyst of the Povarov reaction. Thus, the montmorillonitecatalyzed three-component reaction between aldehydes 223, nitrobenzenes 224 and cyclopentadiene (39)  Beifuss and coworkers developed a straightforward procedure for the diastereoselective synthesis of tetrahydroquinolines based on a domino process involving in situ reduction, imine formation and aza-Diels-Alder reaction (Scheme 53a) [141]. Using nitrobenzenes instead of the typical aniline derivatives, the domino process was triggered by in situ reduction of 224 with iron in combination with citric acid as chelating ligand and montmorillonite as catalyst of the Povarov reaction. Thus, the montmorillonite-catalyzed three-component reaction between aldehydes 223, nitrobenzenes 224 and cyclopentadiene (39) in aqueous citric acid at 40 • C, in the presence of iron, gave rise to tetrahydroquinolines 225/226 with high endo-selectivity and high yields. The catalytic method showed a wide substrate scope, with several substituted nitrobenzenes and aromatic, heteroaromatic and aliphatic aldehydes as suitable substrates. Later, the same group established the intramolecular version of this methodology by using ω-unsaturated aldehydes (e.g., 227) as substrates (Scheme 53b) [142]. Under the same catalytic system, diastereomerically pure trans-fused tetrahydrochromano [4,3-b]quinolones 228 were obtained from the onepot domino reduction/imine formation/intramolecular aza-Diels-Alder reaction between nitrobenzenes 224 and ω-unsaturated aldehydes 227, in yields ranging from 69 to 87%. However, higher temperatures (80 • C) and an increased amount of iron (4 equiv) and montmorillonite (10 wt%) were necessary to attain high levels of efficiency. The observed diastereoselectivity was rationalized as resulting from the exo-E-anti transition state 229 in the cyclization step, in which both the C=N bond of the diene and the C=C of the dienophile present E-configuration (Scheme 53b). method showed a wide substrate scope, with several substituted nitrobenzenes and aromatic, heteroaromatic and aliphatic aldehydes as suitable substrates. Later, the same group established the intramolecular version of this methodology by using ω-unsaturated aldehydes (e.g., 227) as substrates (Scheme 53b) [142]. Under the same catalytic system, diastereomerically pure trans-fused tetrahydrochromano [4,3-b]quinolones 228 were obtained from the one-pot domino reduction/imine formation/intramolecular aza-Diels-Alder reaction between nitrobenzenes 224 and ω-unsaturated aldehydes 227, in yields ranging from 69 to 87%. However, higher temperatures (80 °C) and an increased amount of iron (4 equiv) and montmorillonite (10 wt%) were necessary to attain high levels of efficiency. The observed diastereoselectivity was rationalized as resulting from the exo-Eanti transition state 229 in the cyclization step, in which both the C=N bond of the diene and the C=C of the dienophile present E-configuration (Scheme 53b). More recently, a different methodology for preparing spiro(isoxazolo[5,4-b]pyridine-5,5′-pyrimidine) derivatives 232 based on an L-proline-promoted one-pot aza-Diels-Alder reaction in water has been disclosed (Scheme 54) [143]. This method has the advantage of generating in situ the 5-amino-3-methylisoxazole (160a) from readily available 3-Scheme 53. Domino reduction/imine formation/aza-Diels-Alder reaction in water of: (a) nitrobenzenes, aldehydes and cyclopentadiene; (b) nitrobenzenes and ω-unsaturated aldehydes.
More recently, a different methodology for preparing spiro(isoxazolo [5,4-b]pyridine-5,5 -pyrimidine) derivatives 232 based on an L-proline-promoted one-pot aza-Diels-Alder reaction in water has been disclosed (Scheme 54) [143]. This method has the advantage of generating in situ the 5-amino-3-methylisoxazole (160a) from readily available 3-aminocrotononitrile (230) and hydroxylamine hydrochloride (231). Designed experiments were performed and confirmed the formation of isoxazole 160a and Knoevenagel adduct 166 as reaction intermediates. The presence of L-proline seems to be a requirement for attaining high efficiency since carrying out the reaction in its absence led to 232 in decreased yield (29%); however, no information was given regarding the stereochemistry outcome or its role in an eventual asymmetric induction. Kouznetsov and coworkers have reported a green methodology for the preparation of a series of 4-amido-N-yl-2-methyl-tetrahydroquinolines (THQs) based on an acidpromoted domino sequence involving "Mannich-like" reaction/imino-Diels-Alder reaction (Scheme 55) [144]. This ABB' three-component reaction employs one molecule of functionalized aniline 2 and two molecules of cyclic or acyclic N-vinyl amides 233 to furnish the target cis-2,4-disubstituted THQs 235 in high to excellent yield, in acidified water using sodium dodecyl sulfate (SDS) surfactant as catalyst. The proposed mechanism involves a domino process ran in the proximity of the anionic SDS micelle surface, presenting some charged species and protons (NH and H + ), initiated by protonation of 233 followed by reaction with amine 2 to give intermediate 234, which then reacts with the second molecule of 233 to afford the desired products 235. Consequently, the reaction outcome was strongly influenced by the micellar concentration as well as by the pH reaction medium. In fact, no reaction occurred in the absence of SDS or when the pH was higher (e.g., pH 7). The best results were achieved when using a 12 mM SDS concentration and pH 1. Moreover, this protocol has the advantage of using a micellar aqueous catalyst that is biodegradable and can be reused. Using a fluorous micellar system in water, several Diels-Alder reactions between typical dienophiles and dienes proceeded in high yields, with remarkable rate acceleration [145]. For example, 9-methylanthracene (236) underwent [4 + 2] annulation reaction with N-octyl maleimide (55e) to give the corresponding cycloadduct 237 in quantitative yield, after only 10 min at room temperature (Scheme 56a). The reaction media, composed of 100 L-Proline-catalyzed one-pot aza-Diels-Alder reaction in water leading to spiro(isoxazolo [5,4-b]pyridine-5,5 -pyrimidine) derivatives.
Kouznetsov and coworkers have reported a green methodology for the preparation of a series of 4-amido-N-yl-2-methyl-tetrahydroquinolines (THQs) based on an acidpromoted domino sequence involving "Mannich-like" reaction/imino-Diels-Alder reaction (Scheme 55) [144]. This ABB' three-component reaction employs one molecule of functionalized aniline 2 and two molecules of cyclic or acyclic N-vinyl amides 233 to furnish the target cis-2,4-disubstituted THQs 235 in high to excellent yield, in acidified water using sodium dodecyl sulfate (SDS) surfactant as catalyst. The proposed mechanism involves a domino process ran in the proximity of the anionic SDS micelle surface, presenting some charged species and protons (NH and H + ), initiated by protonation of 233 followed by reaction with amine 2 to give intermediate 234, which then reacts with the second molecule of 233 to afford the desired products 235. Consequently, the reaction outcome was strongly influenced by the micellar concentration as well as by the pH reaction medium. In fact, no reaction occurred in the absence of SDS or when the pH was higher (e.g., pH 7). The best results were achieved when using a 12 mM SDS concentration and pH 1. Moreover, this protocol has the advantage of using a micellar aqueous catalyst that is biodegradable and can be reused. Kouznetsov and coworkers have reported a green methodology for the preparation of a series of 4-amido-N-yl-2-methyl-tetrahydroquinolines (THQs) based on an acidpromoted domino sequence involving "Mannich-like" reaction/imino-Diels-Alder reaction (Scheme 55) [144]. This ABB' three-component reaction employs one molecule of functionalized aniline 2 and two molecules of cyclic or acyclic N-vinyl amides 233 to furnish the target cis-2,4-disubstituted THQs 235 in high to excellent yield, in acidified water using sodium dodecyl sulfate (SDS) surfactant as catalyst. The proposed mechanism involves a domino process ran in the proximity of the anionic SDS micelle surface, presenting some charged species and protons (NH and H + ), initiated by protonation of 233 followed by reaction with amine 2 to give intermediate 234, which then reacts with the second molecule of 233 to afford the desired products 235. Consequently, the reaction outcome was strongly influenced by the micellar concentration as well as by the pH reaction medium. In fact, no reaction occurred in the absence of SDS or when the pH was higher (e.g., pH 7). The best results were achieved when using a 12 mM SDS concentration and pH 1. Moreover, this protocol has the advantage of using a micellar aqueous catalyst that is biodegradable and can be reused. Using a fluorous micellar system in water, several Diels-Alder reactions between typical dienophiles and dienes proceeded in high yields, with remarkable rate acceleration [145]. For example, 9-methylanthracene (236) underwent [4 + 2] annulation reaction with N-octyl maleimide (55e) to give the corresponding cycloadduct 237 in quantitative yield, after only 10 min at room temperature (Scheme 56a). The reaction media, composed of 100 Using a fluorous micellar system in water, several Diels-Alder reactions between typical dienophiles and dienes proceeded in high yields, with remarkable rate acceleration [145]. For example, 9-methylanthracene (236) underwent [4 + 2] annulation reaction with N-octyl maleimide (55e) to give the corresponding cycloadduct 237 in quantitative yield, after only 10 min at room temperature (Scheme 56a). The reaction media, composed of 100 mM perfluorohexane (PFH) and lithium perfluorooctanesulfonate (LiFOS)/water (10 mL each), originate a large interfacial area between the fluorous solvent and the water, where the reaction occurs more effectively due to repulsion effects from both media. Furthermore, LiFOS acts not only as a surfactant but also as a supporting electrolyte, enabling the use of electrochemical approaches in the micellar system. Thus, ethyl 3,4-dioxocyclohexa-1,5dienecarboxylate (240), generated electrochemically from ethyl 3,4-dihydroxybenzoate (238), was trapped by dienes (e.g., 239) at the surface of the micelle or at the interface to afford the corresponding Diels-Alder cycloadduct (e.g., 241) in excellent yield (Scheme 56b). The development of new carbocatalysts which are eco-friendly and sustainable has attracted great attention. Owing to their easy preparation from inexpensive graphite, graphene and graphene oxide (GO) have emerged as efficient carbocatalysts for several transformations in organic synthesis, namely the Diels-Alder reaction. De and coworkers have disclosed the GO-promoted Diels-Alder reaction between 9hydroxymethylanthracene (54) and N-substituted maleimides 55 in an aqueous medium at room temperature leading to the corresponding cycloadducts 242 in moderate to excellent yields (Scheme 57) [146]. The catalytic protocol has a wide substrate scope, and the GO catalyst can be easily recovered by centrifugation or filtration and reutilized up to four times without significant loss of activity. A three-step mechanism was proposed involving the initial binding of the hydroxyl groups and the aromatic rings to the GO surface by weak hydrogen bonding and π-π interactions. Subsequently to the product formation, the anthracene moiety loses its planar structure as well as the partial aromaticity leading to the weakness of the π-π interactions and displacement of the product by another molecule of reactant. Experimental calculations were carried out and corroborated the proposed mechanism. Scheme 57. GO-catalyzed Diels-Alder reaction of anthracene derivatives and N-substituted maleimides in water. Scheme 56. Diels-Alder reactions using a fluorous micellar system in water of: (a) 9-methylanthracene and N-octyl maleimide; (b) 3,4-dihydroxybenzoate and 2,3-dimethylbuta-1,3-diene.

Asymmetric Diels-Alder Cycloaddition Reactions
The development of new carbocatalysts which are eco-friendly and sustainable has attracted great attention. Owing to their easy preparation from inexpensive graphite, graphene and graphene oxide (GO) have emerged as efficient carbocatalysts for several transformations in organic synthesis, namely the Diels-Alder reaction. De and coworkers have disclosed the GO-promoted Diels-Alder reaction between 9-hydroxymethylanthracene (54) and N-substituted maleimides 55 in an aqueous medium at room temperature leading to the corresponding cycloadducts 242 in moderate to excellent yields (Scheme 57) [146]. The catalytic protocol has a wide substrate scope, and the GO catalyst can be easily recovered by centrifugation or filtration and reutilized up to four times without significant loss of activity. A three-step mechanism was proposed involving the initial binding of the hydroxyl groups and the aromatic rings to the GO surface by weak hydrogen bonding and π-π interactions. Subsequently to the product formation, the anthracene moiety loses its planar structure as well as the partial aromaticity leading to the weakness of the π-π interactions and displacement of the product by another molecule of reactant. Experimental calculations were carried out and corroborated the proposed mechanism. The development of new carbocatalysts which are eco-friendly and sustainable has attracted great attention. Owing to their easy preparation from inexpensive graphite, graphene and graphene oxide (GO) have emerged as efficient carbocatalysts for several transformations in organic synthesis, namely the Diels-Alder reaction. De and coworkers have disclosed the GO-promoted Diels-Alder reaction between 9hydroxymethylanthracene (54) and N-substituted maleimides 55 in an aqueous medium at room temperature leading to the corresponding cycloadducts 242 in moderate to excellent yields (Scheme 57) [146]. The catalytic protocol has a wide substrate scope, and the GO catalyst can be easily recovered by centrifugation or filtration and reutilized up to four times without significant loss of activity. A three-step mechanism was proposed involving the initial binding of the hydroxyl groups and the aromatic rings to the GO surface by weak hydrogen bonding and π-π interactions. Subsequently to the product formation, the anthracene moiety loses its planar structure as well as the partial aromaticity leading to the weakness of the π-π interactions and displacement of the product by another molecule of reactant. Experimental calculations were carried out and corroborated the proposed mechanism. Scheme 57. GO-catalyzed Diels-Alder reaction of anthracene derivatives and N-substituted maleimides in water.

Asymmetric Diels-Alder Cycloaddition Reactions
Zhang and coworkers reported a rate-accelerating effect in the asymmetric organocatalytic Diels-Alder reactions between α,β-unsaturated aldehydes 40 and

Asymmetric Diels-Alder Cycloaddition Reactions
Zhang and coworkers reported a rate-accelerating effect in the asymmetric organocatalytic Diels-Alder reactions between α,β-unsaturated aldehydes 40 and cyclopentadiene (39), catalyzed by C 2 -symmetric bipyrrolidine 243 and HClO 4 in aqueous reaction medium (Scheme 58) [147]. In contrast with the reactions performed in organic solvents, the reactions carried out in water were completed within only 2-3.5 h, furnishing cycloadducts 244 in high yields with good enantioselectivity and moderate exo-selectivity. Moreover, the catalyst 243. 2HClO 4 could be recovered by diethyl ether extraction and reused directly up to four times while retaining its catalytic activity. DFT calculations and X-ray studies corroborated the proposed mechanism which involves the formation of a C 2 -symmetric diiminium intermediate (e.g., (E,E)-245), with two conjugated iminiums facing each other, corresponding to two Si faces giving rise to the same enantiofacial discrimination in the cycloaddition step. A poly(methylhydrosiloxane) (PMHS)-supported chiral organic catalyst derived from MacMillan's imidazolidin-4-ones (e.g., 246) also has the ability to promote successfully Diels-Alder cycloaddition reactions in aqueous medium with a high degree of enantioselectivity (up to 93% ee), albeit with low exo/endo selectivity (Scheme 59) [148]. The cycloaddition reaction between trans-cinnamaldehyde (40a) and cyclopentadiene (39) was investigated under different catalytic reaction conditions, with higher yields and enantioselectivities being achieved when a preformed PMHS-supported HBF4 salt of 246 was used in water. Nevertheless, it was observed that when using only water as solvent, the catalyst activity decreased dramatically after the second recycle run, whereas a 95:5 acetonitrile:H2O mixture proved to be the ideal solvent system to ensure the recycling of the PMHS-supported catalyst. Scheme 59. Asymmetric Diels-Alder reaction in water promoted by HBF4 salt of PMHS-supported chiral imidazolinone catalyst.
In the same year, Wang and coworkers disclosed a straightforward route to new heterogeneous organocatalysts based on the functionalization of hollow-structured phenylene-bridged periodic mesoporous organosilica (PMO) spheres with MacMillan catalyst and investigated its use in the aforementioned Diels-Alder reaction [149]. The cycloaddition reaction performed in water using 20 mol% of catalyst, in the presence of TFA, led to cycloadducts 244a in excellent overall yield (98%) and high enantiomeric excess (81% for endo-adduct and 81% for exo-adduct). Furthermore, the H-Ph-PMO-Mac catalyst could be reutilized for up to seven catalytic cycles without a significant loss of catalytic activity. A poly(methylhydrosiloxane) (PMHS)-supported chiral organic catalyst derived from MacMillan's imidazolidin-4-ones (e.g., 246) also has the ability to promote successfully Diels-Alder cycloaddition reactions in aqueous medium with a high degree of enantioselectivity (up to 93% ee), albeit with low exo/endo selectivity (Scheme 59) [148]. The cycloaddition reaction between trans-cinnamaldehyde (40a) and cyclopentadiene (39) was investigated under different catalytic reaction conditions, with higher yields and enantioselectivities being achieved when a preformed PMHS-supported HBF 4 salt of 246 was used in water. Nevertheless, it was observed that when using only water as solvent, the catalyst activity decreased dramatically after the second recycle run, whereas a 95:5 acetonitrile:H 2 O mixture proved to be the ideal solvent system to ensure the recycling of the PMHS-supported catalyst. A poly(methylhydrosiloxane) (PMHS)-supported chiral organic catalyst derived from MacMillan's imidazolidin-4-ones (e.g., 246) also has the ability to promote successfully Diels-Alder cycloaddition reactions in aqueous medium with a high degree of enantioselectivity (up to 93% ee), albeit with low exo/endo selectivity (Scheme 59) [148]. The cycloaddition reaction between trans-cinnamaldehyde (40a) and cyclopentadiene (39) was investigated under different catalytic reaction conditions, with higher yields and enantioselectivities being achieved when a preformed PMHS-supported HBF4 salt of 246 was used in water. Nevertheless, it was observed that when using only water as solvent, the catalyst activity decreased dramatically after the second recycle run, whereas a 95:5 acetonitrile:H2O mixture proved to be the ideal solvent system to ensure the recycling of the PMHS-supported catalyst. Scheme 59. Asymmetric Diels-Alder reaction in water promoted by HBF4 salt of PMHS-supported chiral imidazolinone catalyst.
In the same year, Wang and coworkers disclosed a straightforward route to new heterogeneous organocatalysts based on the functionalization of hollow-structured phenylene-bridged periodic mesoporous organosilica (PMO) spheres with MacMillan catalyst and investigated its use in the aforementioned Diels-Alder reaction [149]. The cycloaddition reaction performed in water using 20 mol% of catalyst, in the presence of TFA, led to cycloadducts 244a in excellent overall yield (98%) and high enantiomeric excess (81% for endo-adduct and 81% for exo-adduct). Furthermore, the H-Ph-PMO-Mac catalyst could be reutilized for up to seven catalytic cycles without a significant loss of catalytic activity. In the same year, Wang and coworkers disclosed a straightforward route to new heterogeneous organocatalysts based on the functionalization of hollow-structured phenylenebridged periodic mesoporous organosilica (PMO) spheres with MacMillan catalyst and investigated its use in the aforementioned Diels-Alder reaction [149]. The cycloaddition reaction performed in water using 20 mol% of catalyst, in the presence of TFA, led to cycloadducts 244a in excellent overall yield (98%) and high enantiomeric excess (81% for endo-adduct and 81% for exo-adduct). Furthermore, the H-Ph-PMO-Mac catalyst could be reutilized for up to seven catalytic cycles without a significant loss of catalytic activity.
The "on-water" organocatalyzed [4 + 2] cycloaddition reaction of acyclic enones with nitro dienes and allylidene malononitriles gave access to a plethora of functionalized chiral cyclohexanones, using cinchona alkaloid-based primary amines (e.g., 249 and 252) and benzoic acid as the organocatalytic system (Scheme 60) [150,151]. Thus, unsaturated methyl ketones 247 reacted smoothly with primary amine catalyst 249 in the presence of benzoic acid to give the corresponding enamine, which undergoes an endo [4 + 2] cycloaddition with nitro dienes 248 to yield the corresponding 3,4,5-trisubstituted cyclohexanones 250 in good yield, with good diastereoselectivities and excellent enantioselectivities. The reaction outcome was not significantly affected by the nature and positioning of the aryl substituents of both reactants. Interestingly, mechanistic studies revealed that the kinetic endo-cycloadduct initially formed with an α-nitro-bearing center, epimerized under the reaction conditions to thermodynamically more stable diastereoisomer 250 with a β-nitrobearing center. On the other hand, the use of allylidene malononitriles 251 as dienophiles led to the enantioselective synthesis of cyclohexanones 253 with two stereocenters and an all-carbon quaternary center. The highest enantioselectivity was achieved from the reaction of benzylidene acetone with allylidene malononitrile bearing a nitro-substituted aryl group (82% ee). Moreover, allylidene cyanoacetates were also suitable dienophiles for these transformations. and benzoic acid as the organocatalytic system (Scheme 60) [150,151]. Thus, unsaturated methyl ketones 247 reacted smoothly with primary amine catalyst 249 in the presence of benzoic acid to give the corresponding enamine, which undergoes an endo [4 + 2] cycloaddition with nitro dienes 248 to yield the corresponding 3,4,5-trisubstituted cyclohexanones 250 in good yield, with good diastereoselectivities and excellent enantioselectivities. The reaction outcome was not significantly affected by the nature and positioning of the aryl substituents of both reactants. Interestingly, mechanistic studies revealed that the kinetic endo-cycloadduct initially formed with an α-nitro-bearing center, epimerized under the reaction conditions to thermodynamically more stable diastereoisomer 250 with a β-nitro-bearing center. On the other hand, the use of allylidene malononitriles 251 as dienophiles led to the enantioselective synthesis of cyclohexanones 253 with two stereocenters and an all-carbon quaternary center. The highest enantioselectivity was achieved from the reaction of benzylidene acetone with allylidene malononitrile bearing a nitro-substituted aryl group (82% ee). Moreover, allylidene cyanoacetates were also suitable dienophiles for these transformations. DNA-based hybrid catalysts combine the catalytic power of a metal complex with the unique helical chirality and chemical stability of DNA and have been employed successfully in various asymmetric transformations, namely the asymmetric Diels-Alder reaction. A solid-supported DNA (st-DNA/S1), prepared from purified salmon testes DNA (st-DNA) and ammonium-functionalized silica (S1), has been used in the copper(II)catalyzed Diels-Alder reaction of 2-azachalcone 254a and cyclopentadiene (39) in water (Scheme 61) [152]. The catalytic protocol involves the mixing of a Cu(dmbpy) complex with st-DNA/S1 in a MOPS buffer solution, the subsequent addition of the reactants and the continuous rotation of the reaction mixture at 5 °C for 3 days. The target cycloadduct 255 was obtained with excellent endo-selectivity (endo/exo ratio of 99:1) with 99% conversion and 94% ee. Performing the reaction with unsupported st-DNA led to 255 with a slight increase in the ee (99%) and similar conversion (93%), whereas the controlled experiment using only S1 without st-DNA afforded 255 in low conversion (14%) and neglectable ee (<3%). In addition, the catalyst st-DNA/S1 was recycled and reused for 10 cycles affording conversions above 93% in each cycle and ee's ranging from 88 to 94%, thus demonstrating its utility as a reusable chiral source. DNA-based hybrid catalysts combine the catalytic power of a metal complex with the unique helical chirality and chemical stability of DNA and have been employed successfully in various asymmetric transformations, namely the asymmetric Diels-Alder reaction. A solid-supported DNA (st-DNA/S1), prepared from purified salmon testes DNA (st-DNA) and ammonium-functionalized silica (S1), has been used in the copper(II)-catalyzed Diels-Alder reaction of 2-azachalcone 254a and cyclopentadiene (39) in water (Scheme 61) [152]. The catalytic protocol involves the mixing of a Cu(dmbpy) complex with st-DNA/S1 in a MOPS buffer solution, the subsequent addition of the reactants and the continuous rotation of the reaction mixture at 5 • C for 3 days. The target cycloadduct 255 was obtained with excellent endo-selectivity (endo/exo ratio of 99:1) with 99% conversion and 94% ee. Performing the reaction with unsupported st-DNA led to 255 with a slight increase in the ee (99%) and similar conversion (93%), whereas the controlled experiment using only S1 without st-DNA afforded 255 in low conversion (14%) and neglectable ee (<3%). In addition, the catalyst st-DNA/S1 was recycled and reused for 10 cycles affording conversions above 93% in each cycle and ee's ranging from 88 to 94%, thus demonstrating its utility as a reusable chiral source. In another example of bioinspired catalysts, Liskamp and coworkers disclosed the asymmetric copper(II)-promoted Diels-Alder reaction in water using tris-histidinecontaining triazacyclophane (TAC), a scaffold that mimics the structure of the trishistidine triad metal-binding site found in several metalloenzymes (Scheme 62) [153]. Due to their ability to coordinate efficiently with Cu II in water, 2-azachalcone 254a and α,βunsaturated 2-acylimidazole 254b were selected as substrates for the Cu(II)-catalyzed cycloaddition with cyclopentadiene (39). Among the several TAC-based ligands screened, compounds 256 and 257 bearing three D-and L-histidine residues, respectively, directly attached to the TAC scaffold and acetylated α-amino groups, afforded selectively the target products 255 with the highest ee (up to 55%). Using ligand 256, cycloadduct 255 with SS configuration was obtained, whereas ligand 257 induced the selective synthesis of its enantiomer. Moreover, attempts to further improve the enantioselectivity through the insertion of additional amino acid residues on the N-termini of the histidine moieties, as well as between the TAC scaffold and the histidine residues, resulted in significantly decreased ee. Scheme 62. Cu(II)-catalyzed Diels-Alder reaction in water using triazacyclophane-derived ligands.

Total Synthesis
The generation of high structural complexity from simple starting materials through the creation of two C-C bonds, at least two rings and up to four stereoisomers in a single step makes the intramolecular Diels-Alder a powerful synthetic tool in the synthesis of complex natural products such as verrubenzospirolactone, a meroterpenoid isolated from the soft coral Simularia verruca [154][155][156]. The total synthesis of verrubenzospirolactone 262, featuring a pentacyclic structure comprising a spirocyclic butenolide and five contiguous stereocenters, was successfully accomplished in five steps starting from In another example of bioinspired catalysts, Liskamp and coworkers disclosed the asymmetric copper(II)-promoted Diels-Alder reaction in water using tris-histidine-containing triazacyclophane (TAC), a scaffold that mimics the structure of the tris-histidine triad metal-binding site found in several metalloenzymes (Scheme 62) [153]. Due to their ability to coordinate efficiently with Cu II in water, 2-azachalcone 254a and α,β-unsaturated 2acylimidazole 254b were selected as substrates for the Cu(II)-catalyzed cycloaddition with cyclopentadiene (39). Among the several TAC-based ligands screened, compounds 256 and 257 bearing three Dand L-histidine residues, respectively, directly attached to the TAC scaffold and acetylated α-amino groups, afforded selectively the target products 255 with the highest ee (up to 55%). Using ligand 256, cycloadduct 255 with SS configuration was obtained, whereas ligand 257 induced the selective synthesis of its enantiomer. Moreover, attempts to further improve the enantioselectivity through the insertion of additional amino acid residues on the N-termini of the histidine moieties, as well as between the TAC scaffold and the histidine residues, resulted in significantly decreased ee. In another example of bioinspired catalysts, Liskamp and coworkers disclosed the asymmetric copper(II)-promoted Diels-Alder reaction in water using tris-histidinecontaining triazacyclophane (TAC), a scaffold that mimics the structure of the trishistidine triad metal-binding site found in several metalloenzymes (Scheme 62) [153]. Due to their ability to coordinate efficiently with Cu II in water, 2-azachalcone 254a and α,βunsaturated 2-acylimidazole 254b were selected as substrates for the Cu(II)-catalyzed cycloaddition with cyclopentadiene (39). Among the several TAC-based ligands screened, compounds 256 and 257 bearing three D-and L-histidine residues, respectively, directly attached to the TAC scaffold and acetylated α-amino groups, afforded selectively the target products 255 with the highest ee (up to 55%). Using ligand 256, cycloadduct 255 with SS configuration was obtained, whereas ligand 257 induced the selective synthesis of its enantiomer. Moreover, attempts to further improve the enantioselectivity through the insertion of additional amino acid residues on the N-termini of the histidine moieties, as well as between the TAC scaffold and the histidine residues, resulted in significantly decreased ee. Scheme 62. Cu(II)-catalyzed Diels-Alder reaction in water using triazacyclophane-derived ligands.

Total Synthesis
The generation of high structural complexity from simple starting materials through the creation of two C-C bonds, at least two rings and up to four stereoisomers in a single step makes the intramolecular Diels-Alder a powerful synthetic tool in the synthesis of complex natural products such as verrubenzospirolactone, a meroterpenoid isolated from the soft coral Simularia verruca [154][155][156]. The total synthesis of verrubenzospirolactone 262, featuring a pentacyclic structure comprising a spirocyclic butenolide and five contiguous stereocenters, was successfully accomplished in five steps starting from

Total Synthesis
The generation of high structural complexity from simple starting materials through the creation of two C-C bonds, at least two rings and up to four stereoisomers in a single step makes the intramolecular Diels-Alder a powerful synthetic tool in the synthesis of complex natural products such as verrubenzospirolactone, a meroterpenoid isolated from the soft coral Simularia verruca [154][155][156]. The total synthesis of verrubenzospirolactone 262, featuring a pentacyclic structure comprising a spirocyclic butenolide and five contiguous stereocenters, was successfully accomplished in five steps starting from readily available methylhydroquinone (258) and citral (259) (Scheme 63a) [157]. The key step of this synthesis involved an unusual intramolecular Diels-Alder reaction between the 2H-chromene and diene moieties of conjugated triene (Z)-261 which upon heating "on-water" at 50 • C afforded verrubenzospirolactone 262 in 61% yield, along with its C9 epimer 263 in 10% yield. The former is the intramolecular Diels-Alder cycloadduct obtained from the scis conformation of (Z)-261 via an exo transition state, whereas the latter resulted from the exo intramolecular Diels-Alder reaction of the s-cis conformation of (E)-261. Starting from a more functionalized aldehyde bearing a triene unit, a quadruple cascade reaction consisting of a Knoevenagel condensation/oxa-6π-electrocyclization/Diels-Alder/oxa-Michael sequence was developed, leading to the formation of a 3:1 mixture of hexacycles 265 (epimers at C11) in 46% yield (Scheme 63b). readily available methylhydroquinone (258) and citral (259) (Scheme 63a) [157]. The key step of this synthesis involved an unusual intramolecular Diels-Alder reaction between the 2H-chromene and diene moieties of conjugated triene (Z)-261 which upon heating "on-water" at 50 °C afforded verrubenzospirolactone 262 in 61% yield, along with its C9 epimer 263 in 10% yield. The former is the intramolecular Diels-Alder cycloadduct obtained from the s-cis conformation of (Z)-261 via an exo transition state, whereas the latter resulted from the exo intramolecular Diels-Alder reaction of the s-cis conformation of (E)-261. Starting from a more functionalized aldehyde bearing a triene unit, a quadruple cascade reaction consisting of a Knoevenagel condensation/oxa-6πelectrocyclization/Diels-Alder/oxa-Michael sequence was developed, leading to the formation of a 3:1 mixture of hexacycles 265 (epimers at C11) in 46% yield (Scheme 63b). The total synthesis of natural product delitschiapyrone A, featuring an impressive 6/6/5/7/6 pentacyclic ring system with five contiguous stereocenters, has also been recently disclosed [158]. This natural product was isolated from the fungus Delitschia sp. FL1581 and exhibits cytotoxic activity against several cancer cell lines (IC50: 12.3-35.5 µM). This challenging synthesis involves a seven-step sequence in which the Diels-Alder reaction of juglone derivative 266 with diene 267 plays a crucial role (Scheme 64). The Diels-Alder reaction, followed by concomitant α-ketol rearrangement and cyclic hemiacetalization, proceeded smoothly at 35 °C in water, leading to the desired cycloadduct 270 in 75% yield, with exclusive regioselectivity and stereoselectivity. To rationalize the observed regioand diastereoselectivity, the energies and coefficients of the frontier orbitals of 266 and 267 were calculated and the DFT-optimized structure of the preferred endo transition state of the Diels-Alder reaction was determined. The presence of the hydroxyl of diene 267 seems to be a requirement to attain selectivity in the Diels-Alder reaction since the reaction of 266 with O-acetyl-267 led to a complex mixture. The total synthesis of natural product delitschiapyrone A, featuring an impressive 6/6/5/7/6 pentacyclic ring system with five contiguous stereocenters, has also been recently disclosed [158]. This natural product was isolated from the fungus Delitschia sp. FL1581 and exhibits cytotoxic activity against several cancer cell lines (IC 50 : 12.3-35.5 µM). This challenging synthesis involves a seven-step sequence in which the Diels-Alder reaction of juglone derivative 266 with diene 267 plays a crucial role (Scheme 64). The Diels-Alder reaction, followed by concomitant α-ketol rearrangement and cyclic hemiacetalization, proceeded smoothly at 35 • C in water, leading to the desired cycloadduct 270 in 75% yield, with exclusive regioselectivity and stereoselectivity. To rationalize the observed regio-and diastereoselectivity, the energies and coefficients of the frontier orbitals of 266 and 267 were calculated and the DFT-optimized structure of the preferred endo transition state of the Diels-Alder reaction was determined. The presence of the hydroxyl of diene 267 seems to be a requirement to attain selectivity in the Diels-Alder reaction since the reaction of 266 with O-acetyl-267 led to a complex mixture.

Conclusions
The Diels-Alder reaction remains one of the most commonly employed reactions for the rapid construction of carbocyclic and heterocyclic compounds, including the synthesis of natural products. In this review, the most significant advances on the Diels-Alder reaction in environmentally benign solvent systems were highlighted.
The fast-growing green chemistry research area has driven successful developments on this topic, upgrading this traditional reaction to the present sustainable needs. Notably, high levels of chemical efficiency and selectivity were achieved in most of the described methodologies, with the use of these sustainable solvent media leading to shorter reaction times and simpler workup procedures than the use of conventional organic solvents. Additionally, the Lewis acid catalysis and organocatalysis combined with nonconventional heating methods have broadened the scope of these methodologies. Despite the recent progress, further developments on sustainable enantioselective synthetic approaches are required. The development of highly active catalysts, namely functionalized heterogeneous catalysts with well-defined structures, suitable to a wider range of substrates and solvents, is needed to overcome some of the current challenges. Therefore, innovative strategies for the design of new catalytic systems with enhanced properties can be expected in the near future.