Recent Advances in the Transition-Metal-Free Synthesis of Quinazolines

Quinazolines are a privileged class of nitrogen-containing heterocycles, widely present in a variety of natural products and synthetic chemicals with a broad spectrum of biological and medicinal activities. Owing to their pharmaceutical applications and promising biological value, a variety of synthetic methodologies have been reported for these scaffolds. From the perspective of green and sustainable chemistry, transition-metal-free synthesis provides an alternative method for accessing several biologically active heterocycles. In this review, we summarize the recent progress achieved in the transition-metal-free synthesis of quinazolines and we cover the literature from 2015 to 2022. This aspect is present alongside the advantages, limitations, mechanistic rationalization, and future perspectives associated with the synthetic methodologies.

Moreover, quinazolines are employed as fragments in the functionalized materials [33] and also serve as useful intermediates in fine chemicals [34]. Owing to this biologically active legacy, quinazolines have emerged as synthetic targets in the last few decades. The first example of the synthesis of quinazolines from cyanogen and anthranilic acid was reported by Griess in 1869 [35]. Consequently, several protocols have been developed since then [36][37][38][39]. Recently, transition-metal-free reactions have received considerable attention and are recognized as an indispensable tool in organic synthesis, as they are not only cost-effective but also environmentally friendly. The metal-free methodology compliments metal-mediated reactions by eliminating expensive metal complexes and Moreover, quinazolines are employed as fragments in the functionalized materials [33] and also serve as useful intermediates in fine chemicals [34]. Owing to this biologically active legacy, quinazolines have emerged as synthetic targets in the last few decades. The first example of the synthesis of quinazolines from cyanogen and anthranilic acid was reported by Griess in 1869 [35]. Consequently, several protocols have been developed since then [36][37][38][39]. Recently, transition-metal-free reactions have received considerable attention and are recognized as an indispensable tool in organic synthesis, as they are not only cost-effective but also environmentally friendly. The metal-free methodology compliments metal-mediated reactions by eliminating expensive metal complexes and toxic metal contamination [40]. There are two classical strategies for the construction of the quinazoline skeleton under metal-free conditions: (i) substituted quinazolines can be prepared from easily available ortho-functionalized anilines such as 2-aminobenzylamines and 2-aminobenzoketones; (ii) using N-arylamidines as a substrate, quinazoline derivatives have been developed, in which pre-activation at the ortho-position of the N-aryl ring is not necessary (Figure 2). These methods mainly involve: (A) condensation of 2-aminobenzylamines with aldehydes followed by oxidation with oxidants such as MnO2, DDQ, and sodium hypochlorite [41][42][43]; a reaction between 2-aminobenzylamines with imines in the presence of K2S2O8 as oxidant [44], (B) oxidative cyclization of 2-aminobenzophenones with benzylamines [45]; two-component oxidative decarboxylative amination reaction of 2-aminobenzophe-

Classical methods
Reports from 2015-2022 These methods mainly involve: (A) condensation of 2-aminobenzylamines with aldehydes followed by oxidation with oxidants such as MnO 2 , DDQ, and sodium hypochlorite [41][42][43]; a reaction between 2-aminobenzylamines with imines in the presence of K 2 S 2 O 8 as oxidant [44], (B) oxidative cyclization of 2-aminobenzophenones with benzylamines [45]; two-component oxidative decarboxylative amination reaction of 2-aminobenzophenones with α-amino acid catalyzed by iodine/TBHP [46]; one-pot three-component reaction of 2-aminobenzophenones, aldehyde, and NH 4 OAc in mixtures of maltose-dimethylurea (DMU)-NH 4 Cl [47]; KI-catalyzed three-component reaction of 2-aminobenzophenones, methylarenes, and NH 4 OAc [48]; NS/TBHP-system-catalyzed reaction with NH 4 OAc as a nitrogen source and dimethylacetamide (DMA) as a one carbon synthon [49], (C) intramolecular oxidative cyclization of N-arylated amidines [50], and (D) microwavepromoted synthesis of quinazolines from N-arylamidines and aldehydes [51] (Figure 3). Despite the efficacy of these protocols, they also suffer from inevitable disadvantages such as the use of excessive quantities of dangerous peroxide reagents, toxic solvents, toxic oxidants such as NaOCl, longer reaction times, elevated temperatures, and requiring strong and hazardous oxidizing agents. Consequently, rapid growth has been witnessed in the last few years regarding the metal-free synthesis of quinazolines, and the methods are compiled in this review. Several reviews have been presented on the synthesis and biological activity of quinazolines [52,53]. This review primarily focuses on the recent progress achieved in the transition-metal-free synthesis of quinazolines and covers the literature from 2015 to 2022. In addition, highlighting the advances made so far, we also point out the limitations associated with them. Furthermore, the article is organized based on the substrates used in a chronological order.

From O-Functionalized Anilines/Amines
In the recent years, transition-metal-free intra-or intermolecular oxidative C(sp 3 )-H amination has upsurged as a significant approach for the direct C-N bond formation [54 Moreover, cost-effectiveness, step economy, and less toxicity are the benefits associate with this strategy. Liu et al. (2015) reported a rarely explored carbon source viz., tertiar amines for the C-N bond formation in quinazolines via an iodine-catalyzed C(sp 3 )-H am nation [55]. The tandem reaction of 2-aminobenzophenone 1 and N-methylamines 2 (ca bon source) in the presence of iodine as a catalyst, ammonium chloride as the nitroge source, utilizing molecular oxygen as an oxidant in DMSO at 120 °C for 12 h furnishe quinazolines 3 in 20-98% yields (Scheme 1). Under the optimized conditions, aromat amines displayed greater reactivity than aliphatic amines. The major advantages of th

From O-Functionalized Anilines/Amines
In the recent years, transition-metal-free intra-or intermolecular oxidative C(sp 3 )-H amination has upsurged as a significant approach for the direct C-N bond formation [54]. Moreover, cost-effectiveness, step economy, and less toxicity are the benefits associated with this strategy. Liu et al. (2015) reported a rarely explored carbon source viz., tertiary amines for the C-N bond formation in quinazolines via an iodine-catalyzed C(sp 3 )-H amination [55]. The tandem reaction of 2-aminobenzophenone 1 and N-methylamines 2 (carbon source) in the presence of iodine as a catalyst, ammonium chloride as the nitrogen source, utilizing molecular oxygen as an oxidant in DMSO at 120 • C for 12 h furnished quinazolines 3 in 20-98% yields (Scheme 1). Under the optimized conditions, aromatic amines displayed greater reactivity than aliphatic amines. The major advantages of this approach involve: peroxide-free, broad substrate scope, operationally simple, oxygen as the green oxidant, metal-free, and easy scalability up to 10 mmol with 90% yield. The plausible reaction mechanism depicted in Scheme 1 suggested that the initial reaction of tetramethylethylenediamine 2 (TMEDA) with iodine generated an aminium iodide A, which then gives an iminium iodide B by the removal of molecular hydrogen iodide. Nucleophilic addition of 1 to B forms an intermediate C by the simultaneous removal of another HI. Later, intermediate E was formed by the nucleophilic addition of ammonia to D. In the last step, E undergoes a tandem condensation-oxidation to provide the desired product 3. Simultaneously, the I2/I catalytic cycle is completed in the form of iodine regeneration via the oxidation of in situ generated HI by oxygen.
Likewise, Bhanage et al. (2016) disclosed a green and sustainable method for the construction of 2-arylquinazolines 6 from 2-aminobenzylamine 4 and N-mono substituted benzylamines 5 in the presence of molecular iodine at 80 °C for 5 h under O2 balloon (Scheme 2) [56]. The optimized reaction conditions worked well for a variety of substrates The plausible reaction mechanism depicted in Scheme 1 suggested that the initial reaction of tetramethylethylenediamine 2 (TMEDA) with iodine generated an aminium iodide A, which then gives an iminium iodide B by the removal of molecular hydrogen iodide. Nucleophilic addition of 1 to B forms an intermediate C by the simultaneous removal of another HI. Later, intermediate E was formed by the nucleophilic addition of ammonia to D. In the last step, E undergoes a tandem condensation-oxidation to provide the desired product 3. Simultaneously, the I 2 /I catalytic cycle is completed in the form of iodine regeneration via the oxidation of in situ generated HI by oxygen.
Likewise, Bhanage et al. (2016) disclosed a green and sustainable method for the construction of 2-arylquinazolines 6 from 2-aminobenzylamine 4 and N-mono substituted benzylamines 5 in the presence of molecular iodine at 80 • C for 5 h under O 2 balloon (Scheme 2) [56]. The optimized reaction conditions worked well for a variety of substrates including electron-donating and electron-withdrawing groups and provided quinazolines 6 in 56-90% yields. Additive-free, solvent-free, transition-metal-free, utilizing oxygen as the green oxidant, shorter reaction times, and simple operation conditions are the major benefits of this approach. An insight into the reaction mechanism as shown in Scheme 2 suggested that the generation of the radical intermediate initiated the reaction, followed by the formation of imine B. Later, imine B reacted with 2-aminobenzylamine 4 to form intermediates C, D, and E successively. In the last step, E undergoes dehydrogenative aromatization to afford the desired product 6. Simultaneously, iodine is regenerated by the reaction of HI with oxygen.
In  An insight into the reaction mechanism as shown in Scheme 2 suggested that the generation of the radical intermediate initiated the reaction, followed by the formation of imine B. Later, imine B reacted with 2-aminobenzylamine 4 to form intermediates C, D, and E successively. In the last step, E undergoes dehydrogenative aromatization to afford the desired product 6. Simultaneously, iodine is regenerated by the reaction of HI with oxygen.
In the same year, Sen et al.  The plausible mechanism proposed by the authors is presented in Scheme 3. The initial attack of nitrogen in intermediate A on the iodine center of IBX, followed by reduction generated the dihydroquinazoline C. Similarly, attack by the nitrogen in dihydroquinazoline C on IBX afforded quinazoline 8 via an intermediate D.
Hypervalent iodine reagents provide a metal-free reaction condition which is essential in the field of medicinal chemistry for the synthesis of pharmacologically important heterocycles. One such example is iodobenzene diacetate (PIDA). Less toxic effect and easy availability made the oxidant be used widely in chemical transformations [58]. Das et al. (2017) disclosed an interesting approach for the synthesis of 2-substitued quinazolines 13 by the reaction of 2-aminobenzylamine 4 with a variety of aldehydes 9, nitriles 10, aliphatic/aryl amines 11, and aliphatic/aryl alcohols 12 in the presence of PIDA as the key reagent, dichloromethane as the solvent, at room temperature for 0.7-1.3 h (Scheme 4) [59]. In the case of alcohols 12 and nitriles 10, catalytic amounts of molecular iodine and zinc chloride, respectively, were employed to facilitate the reaction. A diverse range of aliphatic, aryl, or heteroaryl groups afforded 2-substitued quinazolines 15 in 76-98% yields. The major advantages of this strategy included: (a) readily available starting materials, (b) broad substrate scope, (c) employing a common oxidant for different substrates, (d) mild reaction conditions, (e) absence or presence of additives, and (f) productselective reaction with no side products. The plausible mechanism proposed by the authors is presented in Scheme 3. The initial attack of nitrogen in intermediate A on the iodine center of IBX, followed by reduction generated the dihydroquinazoline C. Similarly, attack by the nitrogen in dihydroquinazoline C on IBX afforded quinazoline 8 via an intermediate D.
Hypervalent iodine reagents provide a metal-free reaction condition which is essential in the field of medicinal chemistry for the synthesis of pharmacologically important heterocycles. One such example is iodobenzene diacetate (PIDA). Less toxic effect and easy availability made the oxidant be used widely in chemical transformations [58]. Das et al. (2017) disclosed an interesting approach for the synthesis of 2-substitued quinazolines 13 by the reaction of 2-aminobenzylamine 4 with a variety of aldehydes 9, nitriles 10, aliphatic/aryl amines 11, and aliphatic/aryl alcohols 12 in the presence of PIDA as the key reagent, dichloromethane as the solvent, at room temperature for 0.7-1.3 h (Scheme 4) [59]. In the case of alcohols 12 and nitriles 10, catalytic amounts of molecular iodine and zinc chloride, respectively, were employed to facilitate the reaction. A diverse range of aliphatic, aryl, or heteroaryl groups afforded 2-substitued quinazolines 15 in 76-98% yields. The major advantages of this strategy included: (a) readily available starting materials, (b) broad substrate scope, (c) employing a common oxidant for different substrates, (d) mild The proposed mechanism as depicted in Scheme 5 suggested that the tween 2-aminobenzylamine 4 and aldehyde 9 resulted in the generation of A. A upon reaction with PIDA led to the formation of intermediate B. Eli lowed by the attack with another molecule of PIDA afforded the desired pr termediates C and D. Oxidation of arylamine 11 and arylalcohol 12 derivative ence of PIDA and PIDA/I2, respectively, generated the corresponding aldeh hydes 9 then underwent a similar course of mechanism to furnish quinazol case of nitriles 10, coordination of ZnCl2 with the cyano group [60] provided diate E, which then liberates ammonia in the presence of ZnCl2 to form int Quinazoline 13 is formed in the subsequent steps by following a similar m detailed earlier. The proposed mechanism as depicted in Scheme 5 suggested that the reaction between 2-aminobenzylamine 4 and aldehyde 9 resulted in the generation of intermediate A. A upon reaction with PIDA led to the formation of intermediate B. Elimination followed by the attack with another molecule of PIDA afforded the desired product via intermediates C and D. Oxidation of arylamine 11 and arylalcohol 12 derivatives in the presence of PIDA and PIDA/I 2 , respectively, generated the corresponding aldehydes 9. Aldehydes 9 then underwent a similar course of mechanism to furnish quinazoline 13. In the case of nitriles 10, coordination of ZnCl 2 with the cyano group [60] provided the intermediate E, which then liberates ammonia in the presence of ZnCl 2 to form intermediate C. Quinazoline 13 is formed in the subsequent steps by following a similar mechanism as detailed earlier. Molecular iodine, a mild Lewis acidic reagent, is known to be an established catalyst in organic reactions. It performs several synthetic transformations such as Michael addition, iodination, oxidation, Prins-related reactions, protection-deprotection of functional groups, and functionalization of alcohols [61]. In spite of the recently reported transitionmetal-free protocols for the functionalization of benzylic sp 3 C-H bonds, there remains a need to develop new strategies for the synthesis of 2-arylquinazolines by overcoming the limitations of previous reports. In this connection, Bhanage et al. (2018) documented a green and sustainable approach for the synthesis of quinazolines via benzylic sp 3 C-H bond amination [62]. The reaction of 2-aminobenzophenones 1 with aryl amines 5 catalyzed by molecular iodine under O2 atmosphere at 130 °C for 3-8 h afforded 2-ar-Scheme 5. PIDA-mediated reaction mechanism for the synthesis of quinazolines. Molecular iodine, a mild Lewis acidic reagent, is known to be an established catalyst in organic reactions. It performs several synthetic transformations such as Michael addition, iodination, oxidation, Prins-related reactions, protection-deprotection of functional groups, and functionalization of alcohols [61]. In spite of the recently reported transition-metal-free protocols for the functionalization of benzylic sp 3  . Broad substrate scope, use of oxygen as the green oxidant, additive-and solvent-free conditions, and lack of aqueous workup are the major benefits of this protocol. Aliphatic and unsaturated amines failed to form the desired product, and this remains the only limitation associated with this strategy. ylquinazolines 15 in 68-92% yields (Scheme 6). Furthermore, the reaction of 2-aminobenzyl alcohol 14 and benzylamine 5 in the presence of molecular iodine under O2 at 130 °C for 15 h delivered 2-arylquinazolines 15 in 49-68% yields (Scheme 6). Broad substrate scope, use of oxygen as the green oxidant, additive-and solvent-free conditions, and lack of aqueous workup are the major benefits of this protocol. Aliphatic and unsaturated amines failed to form the desired product, and this remains the only limitation associated with this strategy. Scheme 6. Molecular-iodine-catalyzed synthesis of quinazolines.
In the same year, Das et al. (2018) developed an oxidant-, base-, and metal-free approach for the synthesis of quinazolines by the reaction of 2-aminobenzylamine 4 with oxalic acid dihydrate or malonic acid in 1,4-dioxane at 120 °C for 6 h via an in situ condensation and oxidation process [63]. Quinazoline 16 and 2-methylquinazoline 17 were obtained in 75-85% yields (Scheme 7). Utilizing oxalic acid dihydrate as the in situ C1 source, easy handling, atom economy, and greener reaction conditions are the merits of this protocol. In the same year, Das et al. (2018) developed an oxidant-, base-, and metal-free approach for the synthesis of quinazolines by the reaction of 2-aminobenzylamine 4 with oxalic acid dihydrate or malonic acid in 1,4-dioxane at 120 • C for 6 h via an in situ condensation and oxidation process [63]. Quinazoline 16 and 2-methylquinazoline 17 were obtained in 75-85% yields (Scheme 7). Utilizing oxalic acid dihydrate as the in situ C1 source, easy handling, atom economy, and greener reaction conditions are the merits of this protocol. ylquinazolines 15 in 68-92% yields (Scheme 6). Furthermore, the reaction of 2-aminob zyl alcohol 14 and benzylamine 5 in the presence of molecular iodine under O2 at 130 for 15 h delivered 2-arylquinazolines 15 in 49-68% yields (Scheme 6). Broad substr scope, use of oxygen as the green oxidant, additive-and solvent-free conditions, and l of aqueous workup are the major benefits of this protocol. Aliphatic and unsatura amines failed to form the desired product, and this remains the only limitation associa with this strategy. Scheme 6. Molecular-iodine-catalyzed synthesis of quinazolines.
In the same year, Das et al. (2018) developed an oxidant-, base-, and metal-free proach for the synthesis of quinazolines by the reaction of 2-aminobenzylamine 4 w oxalic acid dihydrate or malonic acid in 1,4-dioxane at 120 °C for 6 h via an in situ c densation and oxidation process [63]. Quinazoline 16 and 2-methylquinazoline 17 w obtained in 75-85% yields (Scheme 7). Utilizing oxalic acid dihydrate as the in situ source, easy handling, atom economy, and greener reaction conditions are the merits this protocol.  [64]. A variety of electron-donating and electronwithdrawing groups on the substrates delivered quinazolines 19 in 43-81% yields under optimized reaction conditions. The important uses of this synthesis method include: readily available substrates, green and renewable solvent, isolation of products by simple crystallization, formation of benign by-product (NaCl or NaBr), chemical oxidant or additive-free conditions, and avoiding huge solvent-consuming work-up procedures. withdrawing groups on the substrates delivered quinazolines 19 in 43-81% yields under optimized reaction conditions. The important uses of this synthesis method include: readily available substrates, green and renewable solvent, isolation of products by simple crystallization, formation of benign by-product (NaCl or NaBr), chemical oxidant or additivefree conditions, and avoiding huge solvent-consuming work-up procedures. The reaction mechanism outlined in Scheme 8 suggest that the initial base-promoted intermolecular substitution of α,α,α-trihalotoluene 18 by 2-aminobenzylamine 4 led to the generation of intermediate A. Later, base-mediated intramolecular substitution followed by elimination formed the intermediate C, which upon oxidation afforded the desired product, quinazoline 19.  [65]. Under the optimized conditions, a wide range of electron-donating and electron-withdrawing groups present on isothiocyanate 20 and 2-aminobenzophenone 1 offered the corresponding N,4-disubstitued quinazolin-2-amines 21 in 87-95% yields. Moreover, meta and ortho-substituted 2-aminoaryl ketones 1 did not tolerate the established conditions due to the steric effect and this remains a drawback to this strategy. Readily available inexpensive substrates, operational simplicity, shorter reaction times, and excellent yields are the key benefits of this methodology.
tolerate the established conditions due to the steric effect and this remains a drawback to this strategy. Readily available inexpensive substrates, operational simplicity, shorter reaction times, and excellent yields are the key benefits of this methodology.
The plausible mechanism is shown in Scheme 9. Initially, 2-aminobenzophenone 1 undergoes condensation with phenylisothiocyanate 20 to afford the thiourea intermediate A. Then, A reacts with ammonium acetate to form intermediate B, which upon intramolecular attack of the imine NH group onto the thiocarbonyl carbon with concomitant trapping of S anion resulted in the generation of cyclized product C. Aromatization of C delivered the desired product 21 with subsequent removal of S and hydrogen iodide. Hydrogen peroxide has emerged as an ideal oxidant for liquid-phase green chemistry owing to its non-toxic, atom efficient, and environmentally benign properties [66]. The plausible mechanism is shown in Scheme 9. Initially, 2-aminobenzophenone 1 undergoes condensation with phenylisothiocyanate 20 to afford the thiourea intermediate A.

NCS
Then, A reacts with ammonium acetate to form intermediate B, which upon intramolecular attack of the imine NH group onto the thiocarbonyl carbon with concomitant trapping of S anion resulted in the generation of cyclized product C. Aromatization of C delivered the desired product 21 with subsequent removal of S and hydrogen iodide.
Hydrogen peroxide has emerged as an ideal oxidant for liquid-phase green chemistry owing to its non-toxic, atom efficient, and environmentally benign properties [66]. Furthermore, hydrogen peroxide oxidant usually does not require temperatures over 100 • C to carry out oxidation transformations. Phan et al. (2020) presented hydrogen-peroxide-mediated one-pot three-component reaction of 2-aminoaryl ketones 1, aldehydes 22, and ammonium acetate as the nitrogen source for the efficient synthesis of 2,4-substituted quinazolines 23. The transformation proceeded readily in the presence of hydrogen peroxide as an oxidant and DMSO as the solvent under air at 60 • C for 6 h (Scheme 10) [67]. The highlighted benefits of this approach are: readily available and atom-efficient H 2 O 2 , mild reaction conditions, transition-metal-free conditions, and broad substrate scope. Under the optimized conditions, various 2-aminobenzophenones 1 coupled with aromatic, heteroaromatic, and aliphatic aldehydes 22 and delivered the corresponding products 23 in 61-89% yields. This is the first report utilizing hydrogen peroxide as the green oxidant for the synthesis of 2,4-substituted quinazolines 23.
Molecules 2023, 28, x FOR PEER REVIEW 13 of 30 mild reaction conditions, transition-metal-free conditions, and broad substrate scope. Under the optimized conditions, various 2-aminobenzophenones 1 coupled with aromatic, heteroaromatic, and aliphatic aldehydes 22 and delivered the corresponding products 23 in 61-89% yields. This is the first report utilizing hydrogen peroxide as the green oxidant for the synthesis of 2,4-substituted quinazolines 23.
The proposed pathway for the transformation was shown in Scheme 10. In the first step, ammonium acetate was decomposed to ammonia and acetic acid upon heating. Later, condensation between 2-aminoacetophenone 1 with NH3 generated an imine intermediate A. Subsequent condensation between the amino group of A with aldehyde 22 followed by nucleophilic cyclization provided the dihydroquinazoline intermediate B.
In the presence of H2O2 and DMSO, intermediate B was rapidly oxidized to furnish the final product, quinazoline 23. Hexamethyldisilazane (HMDS) is a commercially available stable reagent employed for the silylation reactions to increase the silylating power by utilizing several catalysts [68]. Wang et al. (2020) developed an efficient and mild synthetic route for the facile syn-thesis of substituted quinazolines. The reaction between 2-aminobenzophenones 1 and benzaldehydes 22 in the presence of catalytic trimethylsilyl trifluoromethanesulfonate (TMSOTf) and HMDS in which gaseous ammonia was formed in situ under neat, and microwave irradiation at 150 • C for 0.5 h, delivered substituted quinazolines 24 in 81-94% yields (Scheme 11) [69]. An array of aromatic benzaldehydes 22 substituted with electron-donating and electron-withdrawing groups and heterocyclic carbaldehydes were well tolerated to afford the corresponding quinazolines 24. Moreover, the structures of quinazolines 24 were also confirmed by single-crystal X-ray crystallography. Absence of unnecessary waste due to conventional reaction conditions viz., microwave irradiation, shorter reaction times, gram-scale synthesis with 90-91% yields, broad substrate scope, and good to excellent yields are the merits of this protocol.  [69]. An array of aromatic benzaldehydes 22 substituted with electrondonating and electron-withdrawing groups and heterocyclic carbaldehydes were well tolerated to afford the corresponding quinazolines 24. Moreover, the structures of quinazolines 24 were also confirmed by single-crystal X-ray crystallography. Absence of unnecessary waste due to conventional reaction conditions viz., microwave irradiation, shorter reaction times, gram-scale synthesis with 90-91% yields, broad substrate scope, and good to excellent yields are the merits of this protocol.  Among the biological cascade systems, chemoenzymatic synthesis methods have drawn considerable attention by the integration of biocatalysis with the versatile reactivity of chemocatalysis [70]. Noteworthy advantages of the chemoenzymatic cascade process include: cost-effectiveness, simple operation conditions, improved selectivity, omitting isolation and purification of intermediates, lower waste generation, and higher reaction yields. In this connection, Zhu et al. (2022) reported the first example of the chemoenzymatic synthesis of quinazolines [71]. The condensation reaction of 2-aminobenzylamine 4 and benzyl alcohol 25 in the presence of the HLADH-SBFA catalytic system and maintaining the pH 9.0 by CHES buffer, under air at 30 • C for 24 h, furnished 2-phenylquinazoline 26 in 73% yields (Scheme 12). In this reaction, synthetic bridged flavin analog (SBFA) performed regeneration of both NAD(P) + and the cofactor during the alcohol dehydrogenase (ADH)-catalyzed process of alcohol to aldehyde. HLADH was used as a biocatalyst and SBFA served as a bifunctional chemocatalyst. Mild reaction conditions, employing bifunctional organocatalyst SBFA, and utilizing O 2 as an external oxidant, serve as a green and sustainable alternatives in this strategy. The plausible mechanism, as shown in Scheme 11, indicated that in the initial step, the TMSOTf and HMDS system could form a complex A with the liberation of the triflate anion. The complex A reacts with benzaldehyde 22 to generate an oxonium intermediate B.
Intermediate C was then formed by the intermolecular addition of 2-aminobenzophenone 1 with B. Deprotonation of intermediate D mediated by HMDS resulted in intermediate E. Simultaneous reaction between complex F and TMSOH led to the silylated product TMSOTMS ether and complex G, which upon further transformation, liberated gaseous ammonia by triflate anion. At the same time, TMSOTf was regenerated. Later, intermediate E underwent imination followed by oxidation with in situ ammonia, producing intermediate H. Finally, microwave irradiation of H furnished the desired product quinazoline 24.
Among the biological cascade systems, chemoenzymatic synthesis methods have drawn considerable attention by the integration of biocatalysis with the versatile reactivity of chemocatalysis [70]. Noteworthy advantages of the chemoenzymatic cascade process include: cost-effectiveness, simple operation conditions, improved selectivity, omitting isolation and purification of intermediates, lower waste generation, and higher reaction yields. In this connection, Zhu et al. (2022) reported the first example of the chemoenzymatic synthesis of quinazolines [71]. The condensation reaction of 2-aminobenzylamine 4 and benzyl alcohol 25 in the presence of the HLADH-SBFA catalytic system and maintaining the pH 9.0 by CHES buffer, under air at 30 °C for 24 h, furnished 2-phenylquinazoline 26 in 73% yields (Scheme 12). In this reaction, synthetic bridged flavin analog (SBFA) performed regeneration of both NAD(P) + and the cofactor during the alcohol dehydrogenase (ADH)-catalyzed process of alcohol to aldehyde. HLADH was used as a biocatalyst and SBFA served as a bifunctional chemocatalyst. Mild reaction conditions, employing bifunctional organocatalyst SBFA, and utilizing O2 as an external oxidant, serve as a green and sustainable alternatives in this strategy.  [72]. Broad substrate scope, gram-scale synthesis, clean reaction system, and easy isolation are the noteworthy uses of this approach.
The organocatalytic oxidative reaction mechanism was depicted in Scheme 13. In the first step, benzylamine 5 reacted with 4,6-dihydrosalicyclic acid to form salt A which generated aryloxy radical B and HOO• via hydrogen abstraction by O2. In the next step, intramolecular hydrogen abstraction of the benzyl group led to the formation of radical cation C [73], which then gave imine D under the action of HOO•. Imine D then underwent an amino group exchange reaction with 2-aminobenzylamine 4 in the presence of BF3.Et2O Visible-light photocatalysis has received considerable attention owing to its ability to carry out redox catalysis via a single electron transfer process under mild conditions. Le et al. (2022) synthesized quinazolines by the condensation of 2-aminobenzylamines 4 and α-ketoacids 28 followed by blue-light LED irradiation at room temperature. The reaction of 2-aminobenzylamines 4 and α-ketoacids 28 in the presence of an organic dye photocatalyst, Rose Bengal, in DMF under air in blue-light LED irradiation at room temperature for 16 h gave the corresponding quinazolines 29 in 26-88% yields (Scheme 14) [74]. Transition-metal-free, additive-free, external-oxidizing-agent-free, and simple and mild reaction conditions made this a green and environmentally friendly process. A variety of electron-donating, electron-withdrawing, electrically neutral, and heterocyclic substituents on α-ketoacids worked well under the optimized conditions. The organocatalytic oxidative reaction mechanism was depicted in Scheme 13. In the first step, benzylamine 5 reacted with 4,6-dihydrosalicyclic acid to form salt A which generated aryloxy radical B and HOO• via hydrogen abstraction by O 2 . In the next step, intramolecular hydrogen abstraction of the benzyl group led to the formation of radical cation C [73], which then gave imine D under the action of HOO•. Imine D then underwent an amino group exchange reaction with 2-aminobenzylamine 4 in the presence of BF 3 .Et 2 O to generate intermediate E. Later, F was formed by the intramolecular cyclization of E, enhanced by BF 3 .Et 2 O. In the last step, oxidative aromatization of F delivered the desired product, 2-arylquinazoline 27.
Visible-light photocatalysis has received considerable attention owing to its ability to carry out redox catalysis via a single electron transfer process under mild conditions. Le et al. (2022) synthesized quinazolines by the condensation of 2-aminobenzylamines 4 and α-ketoacids 28 followed by blue-light LED irradiation at room temperature. The reaction of 2-aminobenzylamines 4 and α-ketoacids 28 in the presence of an organic dye photocatalyst, Rose Bengal, in DMF under air in blue-light LED irradiation at room temperature for 16 h gave the corresponding quinazolines 29 in 26-88% yields (Scheme 14) [74]. Transition-metalfree, additive-free, external-oxidizing-agent-free, and simple and mild reaction conditions made this a green and environmentally friendly process. A variety of electron-donating, electron-withdrawing, electrically neutral, and heterocyclic substituents on α-ketoacids worked well under the optimized conditions. 28

From Amidines and Azirines
Molecular iodine is a less toxic and inexpensive oxidant widely used for the oxidative C-X (X = C, N, O, or S) bond construction from C-H bonds for the synthesis of heterocyclic compounds. In this relation, Chang et al. (2016) reported an I2/KI-promoted oxidative C-C bond formation reaction from C(sp 3 )-H and C(sp 2 )-H bonds from N,N'-disubstituted amidines 30 in the presence of potassium carbonate in DMSO at 100 °C for 4 h to provide quinazolines 31 in 39-99% yields (Scheme 15) [75]. The reaction proceeded smoothly with both electron-donating and electron-withdrawing groups on the N'-phenyl rings and gave the corresponding products 31. Gram-scale synthesis with a 61% yield, readily prepared starting precursors, and broad substrate scope are the merits of this protocol.
The mechanism of oxidative cyclization is depicted in Scheme 15. Initially, the oxidation of N-aryl amidine 30 by molecular iodine in the presence of base K2CO3 led to an imine intermediate B. Next, iodine-mediated iodocyclization of B generated a N-iodo species C with a new C-C bond. Base-promoted deprotonation followed by elimination of one molecule of HI, delivered the quinazoline 31.   [75]. The reaction proceeded smoothly with both electron-donating and electron-withdrawing groups on the N'-phenyl rings and gave the corresponding products 31. Gram-scale synthesis with a 61% yield, readily prepared starting precursors, and broad substrate scope are the merits of this protocol.  [76]. The major advantages of this reaction include: lower catalyst loading, improved efficacy of reaction, and tolerating a wide range of functional groups in substrates.

From Amidines and Azirines
The plausible reaction mechanism was demonstrated in more than one pathway (Scheme 16) [77]. In the absence of Rose Bengal, CBr4 was cracked into CBr3 radical and Br radical under visible-light irradiation [78]. CBr3 radical abstracted a hydrogen atom from another molecule of benzimidamide to yield α-amino radical intermediate A, which then entered the radical chain process with CBr4 to give iminium ion C. Intramolecular Friedel-Craft reaction of C generated an intermediate D, which upon dehydrogenation followed by aromatization delivered the desired product 32. In another pathway, quenching of visible-light-excited Rose Bengal (RB*) by benzimidamide led to the formation of Rose Bengal radical anion (RB•−) and radical cation B. The photoredox cycle was completed by the formation of a superoxide radical anion by the transfer of an electron to CBr4 and regen-Scheme 15. I 2 /KI-promoted oxidative synthesis of quinazolines.
The mechanism of oxidative cyclization is depicted in Scheme 15. Initially, the oxidation of N-aryl amidine 30 by molecular iodine in the presence of base K 2 CO 3 led to an imine intermediate B. Next, iodine-mediated iodocyclization of B generated a N-iodo species C with a new C-C bond. Base-promoted deprotonation followed by elimination of one molecule of HI, delivered the quinazoline 31.
In the same year, Tang et al. (2016) disclosed a fast catalytic synthesis of multisubstituted quinazolines from amidines via visible-light-mediated oxidative C(sp 3 )-C(sp 2 ) bond formation. Metal-free oxidative coupling of amidine 30 in the presence of Rose Bengal as a photoredox organocatalyst, CBr 4 as an oxidant, and K 2 CO 3 as the base, in DMSO as the solvent at 100 • C under 18 W fluorescent lamp as the visible-light source provided quinazolines 32 in 30-96% yields (Scheme 16) [76]. The major advantages of this reaction include: lower catalyst loading, improved efficacy of reaction, and tolerating a wide range of functional groups in substrates. An interesting approach was developed by Levin et al. (2022) for the construction of quinazoline scaffolds by the selective cleavage of the N-N bond of the indazole core 33 [79]. This chlorodiazirine-34-mediated reaction provides unified access to quinazolines 35 in the presence of sodium carbonate and methyl tert-butyl ether (MtBE) at 60 °C for 12 h (Scheme 17). Indazoles 33 were tolerant towards a wide range of alkyl substitutions. Moreover, free alcohol, thiophene, and halogen groups substituted in various positions also gave quinazolines 35 in 30-80% yields. The two major limitations associated with this strategy include: (a) substrates with less solubility in refluxing MtBE displayed poor reactivity, and (b) nucleophilicity of diazole was deactivated due to inductive withdrawal and precludes productive reactivity. The plausible reaction mechanism was demonstrated in more than one pathway (Scheme 16) [77]. In the absence of Rose Bengal, CBr 4 was cracked into CBr 3 radical and Br radical under visible-light irradiation [78]. CBr 3 radical abstracted a hydrogen atom from another molecule of benzimidamide to yield α-amino radical intermediate A, which then entered the radical chain process with CBr 4 to give iminium ion C. Intramolecular Friedel-Craft reaction of C generated an intermediate D, which upon dehydrogenation followed by aromatization delivered the desired product 32. In another pathway, quenching of visible-light-excited Rose Bengal (RB*) by benzimidamide led to the formation of Rose Bengal radical anion (RB•−) and radical cation B. The photoredox cycle was completed by the formation of a superoxide radical anion by the transfer of an electron to CBr 4 and regeneration of Rose Bengal. Furthermore, the radical cation B gave up a hydrogen atom to the radical anion to generate CBr 3 radical, bromide anion, and radical intermediate A. The CBr 3 radical abstracted a hydrogen atom from radical cation B and formed iminium ion C, in another pathway.
An interesting approach was developed by Levin et al. (2022) for the construction of quinazoline scaffolds by the selective cleavage of the N-N bond of the indazole core 33 [79]. This chlorodiazirine-34-mediated reaction provides unified access to quinazolines 35 in the presence of sodium carbonate and methyl tert-butyl ether (MtBE) at 60 • C for 12 h (Scheme 17). Indazoles 33 were tolerant towards a wide range of alkyl substitutions. Moreover, free alcohol, thiophene, and halogen groups substituted in various positions also gave quinazolines 35 in 30-80% yields. The two major limitations associated with this strategy include: (a) substrates with less solubility in refluxing MtBE displayed poor reactivity, and (b) nucleophilicity of diazole was deactivated due to inductive withdrawal and precludes productive reactivity.

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Scheme 17. Chlorodiazirine-mediated reaction for the synthesis of quinazolines.

From Nitriles
Liu et al. (2017) reported a (2+2+2) modular synthesis of multi-substituted quinazolines by the direct reaction of two equivalents of nitriles 36 with aryldiazonium salts 37. The reaction of nitriles 36 and aryldiazonium tetrafluoroborate 37 at 110 °C for 3 h provided quinazolines 38 in 11-73% yields (Scheme 18) [80]. Under the optimized conditions, several aryldiazonium tetrafluoroborates 37 with electron-donating and electronwithdrawing groups at different positions in the ring were reacted smoothly to afford the corresponding products 38. Similarly, ortho-or para-substituted phenyldiazonium salts 37 gave quinazolines in good yields with the exception of nitro substituent. Moreover, aliphatic, aromatic, and heteroaromatic nitriles 36 served as suitable substrates for this annulation. Readily available substrates, shorter reaction times, one-pot, neat and metal-free conditions, gram-scale synthesis with 74% yields, flexibility in substitution patterns, atom-efficient, and easy handling procedures are the benefits of this strategy.
The authors proposed that the N-arylnitrilium ion A was generated in situ by the reaction of aryldiazonium salt 37 and nitrile 36. The N-arylnitrilium ion A undergoes a further reaction with another nitrile moiety 36 via tandem addition/electrophilic cyclization to furnish 2,4-disubstituted quinazolines 38 in an atom-economic way (Scheme 18). Scheme 17. Chlorodiazirine-mediated reaction for the synthesis of quinazolines.

From Nitriles
Liu et al. (2017) reported a (2+2+2) modular synthesis of multi-substituted quinazolines by the direct reaction of two equivalents of nitriles 36 with aryldiazonium salts 37. The reaction of nitriles 36 and aryldiazonium tetrafluoroborate 37 at 110 • C for 3 h provided quinazolines 38 in 11-73% yields (Scheme 18) [80]. Under the optimized conditions, several aryldiazonium tetrafluoroborates 37 with electron-donating and electron-withdrawing groups at different positions in the ring were reacted smoothly to afford the corresponding products 38. Similarly, orthoor para-substituted phenyldiazonium salts 37 gave quinazolines in good yields with the exception of nitro substituent. Moreover, aliphatic, aromatic, and heteroaromatic nitriles 36 served as suitable substrates for this annulation. Readily available substrates, shorter reaction times, one-pot, neat and metal-free conditions, gramscale synthesis with 74% yields, flexibility in substitution patterns, atom-efficient, and easy handling procedures are the benefits of this strategy. In the recent years, reports have shown that the treatment of amines with nitriles in the presence of Lewis acids such as trimethylsilyl iodide (TMSI) led to the in situ generation of amidines [83]. In this regard, Pahari et al. (2018) disclosed the synthesis of 2,4-disubstituted quinazolines 43 in 72-78% yields by the reaction between nitriles 42 and 2aminobenzophenone 1 in the presence of the TMSOTf catalyst under microwave irradiation at 100 °C for 10 min (Scheme 20) [84]. Nitriles 42 activated by the Lewis acid catalyst, TMSOTf, were used as the nitrogen source in this reaction. The significant features of this approach include: single-step, mild and solvent-free conditions, in situ generated amidines, broad substrate scope, one-pot, and shorter reaction times. The reaction mechanism as illustrated in Scheme 7 involves the activation of electron-rich nitriles 42 by coordination with TMSOTf. Later, the nucleophilic attack of amine 1 onto the activated nitrile A generated an amidine intermediate B which then attacks the carbonyl to deliver quinazoline 43 via aromatization. Scheme 19. PTSA/KO t Bu-mediated reaction for the synthesis of quinazolines.
In the recent years, reports have shown that the treatment of amines with nitriles in the presence of Lewis acids such as trimethylsilyl iodide (TMSI) led to the in situ generation of amidines [83]. In this regard, Pahari et al. (2018) disclosed the synthesis of 2,4-disubstituted quinazolines 43 in 72-78% yields by the reaction between nitriles 42 and 2-aminobenzophenone 1 in the presence of the TMSOTf catalyst under microwave irradiation at 100 • C for 10 min (Scheme 20) [84]. Nitriles 42 activated by the Lewis acid catalyst, TMSOTf, were used as the nitrogen source in this reaction. The significant features of this approach include: single-step, mild and solvent-free conditions, in situ generated amidines, broad substrate scope, one-pot, and shorter reaction times. The reaction mechanism as illustrated in Scheme 7 involves the activation of electron-rich nitriles 42 by coordination with TMSOTf. Later, the nucleophilic attack of amine 1 onto the activated nitrile A generated an amidine intermediate B which then attacks the carbonyl to deliver quinazoline 43 via aromatization. Conjugated π-systems with arenes or heteroarenes have gained attention due to their applicability in materials science. On the other hand, the synthesis of π-conjugated molecules under transition-metal-free conditions remains a challenge because of intrinsic mechanistic limitations [85]. In this connection, Jiang et al. (2018) developed a transitionmetal-free chemoselective synthesis of π-conjugated quinazoline-substituted ethenes 46 by the reaction of 2-ethynylanilines 45 and benzonitriles 44 in the presence of KO t Bu and dimethylacetamide(DMA)/toluene (4:1) under air at 110 °C for 2 h (Scheme 21) [86]. Twenty-five derivatives were synthesized in moderate to high yields (31-77% yields). Interestingly, all the synthesized quinazolines 46 displayed a marked luminescence phenomenon. A variety of electron-donating and electron-withdrawing groups underwent the reaction and delivered the quinazolines 46 in a complete (Z)-configuration. Under optimized reaction conditions, unsubstituted and electron-donating-group-substituted benzonitriles 44 failed to give the desired product and this marks a major limitation in this approach.
The mechanism involved the initial deprotonation Conjugated π-systems with arenes or heteroarenes have gained attention due to their applicability in materials science. On the other hand, the synthesis of π-conjugated molecules under transition-metal-free conditions remains a challenge because of intrinsic mechanistic limitations [85]. In this connection, Jiang et al. (2018) developed a transitionmetal-free chemoselective synthesis of π-conjugated quinazoline-substituted ethenes 46 by the reaction of 2-ethynylanilines 45 and benzonitriles 44 in the presence of KO t Bu and dimethylacetamide(DMA)/toluene (4:1) under air at 110 • C for 2 h (Scheme 21) [86]. Twenty-five derivatives were synthesized in moderate to high yields (31-77% yields). Interestingly, all the synthesized quinazolines 46 displayed a marked luminescence phenomenon. A variety of electron-donating and electron-withdrawing groups underwent the reaction and delivered the quinazolines 46 in a complete (Z)-configuration. Under optimized reaction conditions, unsubstituted and electron-donating-group-substituted benzonitriles 44 failed to give the desired product and this marks a major limitation in this approach.
attack of E afforded F. In the last step, the desired product 46 is formed with the elimination of one water molecule from G (Scheme 21). The benzene ring at the 2-position of quinazoline drives the stereoselectivity by forming a stereoregular product.

Scheme 21.
Metal-free chemoselective synthesis of π-conjugated quinazolines. Grignard reagent, and phenylisothiocyanate 20 in the presence of an inexpensive base NaOH and water as a solvent at 80 • C for 1-2 h [87]. The reaction of 2-aminobenzonitrile 47 with aryl magnesium bromide resulted in the formation of ortho-aminoketimine 48 [88]. Later, the reaction of o-aminoketimine 48 with isothiocyanate 20 and NaOH in water provided N,4-substituted quinazolines 49 in 76-91% yields (Scheme 22). The noteworthy advantages of this approach include: broad substrate scope, step economy, operational simplicity, shorter reaction times, good functional group tolerance, easy workup procedure, inexpensive precursors, and using water as an environmentally benign solvent.
Palakodety et al. (2019) documented step economy and sustainable synthesis of substituted quinazolines 49 by utilizing the starting precursor 2-aminobenzonitrile 47, Grignard reagent, and phenylisothiocyanate 20 in the presence of an inexpensive base NaOH and water as a solvent at 80 °C for 1-2 h [87]. The reaction of 2-aminobenzonitrile 47 with aryl magnesium bromide resulted in the formation of ortho-aminoketimine 48 [88]. Later, the reaction of o-aminoketimine 48 with isothiocyanate 20 and NaOH in water provided N,4-substituted quinazolines 49 in 76-91% yields (Scheme 22). The noteworthy advantages of this approach include: broad substrate scope, step economy, operational simplicity, shorter reaction times, good functional group tolerance, easy workup procedure, inexpensive precursors, and using water as an environmentally benign solvent.
The plausible mechanism detailed by the authors is depicted in Scheme 22. In the first step, o-aminoketimine 48 reacts with phenylisothiocyanate 20 to generate the thiourea intermediate A. In the next step, the subsequent intramolecular nucleophilic attack of the amine or imine group on the thiocarbonyl carbon led to the formation of the cyclized product C via N-C bond formation. Aromatization followed by subsequent liberation of S and H2O offered the desired quinazoline 49. Scheme 22. Base-catalyzed synthesis of quinazolines.

Conclusions
Owing to the biologically active legacy, quinazolines have emerged as an important synthetic target in the last few decades. The transition-metal-free approaches in organic transformations are always more economical and complements metal-mediated reactions The plausible mechanism detailed by the authors is depicted in Scheme 22. In the first step, o-aminoketimine 48 reacts with phenylisothiocyanate 20 to generate the thiourea intermediate A. In the next step, the subsequent intramolecular nucleophilic attack of the amine or imine group on the thiocarbonyl carbon led to the formation of the cyclized product C via N-C bond formation. Aromatization followed by subsequent liberation of S and H 2 O offered the desired quinazoline 49.

Conclusions
Owing to the biologically active legacy, quinazolines have emerged as an important synthetic target in the last few decades. The transition-metal-free approaches in organic transformations are always more economical and complements metal-mediated reactions that suffer from drawbacks such as the possibility of toxic metal contamination in the final products, using expensive metal complexes, and the restricted applicability of products as pharmaceuticals, due to metal contamination. Consequently, rapid growth has been witnessed in the last few years in metal-free synthesis methods. Despite the efficacy of the reported protocols, they also suffer from inevitable disadvantages such as the use of excessive quantities of dangerous peroxide reagents, toxic solvents, toxic oxidants, longer reaction times, elevated temperatures, and requiring strong and hazardous oxidizing agents. Moreover, most of them are not solely focused on the development of an efficient approach with improved results viz., product yields, cost-effectiveness, atom-economy, and environmentally benign conditions. Hence, the development of novel synthetic strategies that proceed in a green reaction medium in the presence of benign reagents without the use of metal complexes, reagents, and hazardous organic solvents and also liberating minimum or benign waste are highly desirable.
This review highlights the recent progress achieved in the transition-metal-free synthesis of quinazolines and covers the literature from 2015 to 2022. It is presented alongside the advantages, limitations, and mechanistic rationalization associated with them. As discussed in the review, it is obvious that these strategies have noteworthy benefits such as readily available substrates, mild reaction conditions, broad substrate scopes, good to excellent yields, green conditions, gram-scale synthesis, etc. Furthermore, oxygen or air has been used instead of external toxic oxidants, and water as a green solvent made the strategies remarkable from a green and environmentally friendly point of view. In addition, employing microwave and visible-light irradiation techniques resulted in shorter reaction times and enhanced efficiency of reaction. Moreover, π-conjugated quinazolines displayed marked luminescence phenomena with excellent chemoselectivity. Furthermore, metal-free multicomponent reactions paved the way for the facile synthesis of substituted quinazolines. In spite of the merits achieved so far, some limitations such as prolonged reaction times, limited substrate scopes, and steric effects are also observed. Hence, metalfree methodologies should be developed in the near future, addressing these limitations which are efficient and environmentally benign. We believe the present review article will help researchers working on this fascinating area to construct quinazolines with immense applications in the field of medicinal chemistry.