Monoterpene Thiols: Synthesis and Modifications for Obtaining Biologically Active Substances

Monoterpene thiols are one of the classes of natural flavors that impart the smell of citrus fruits, grape must and wine, black currants, and guava and are used as flavoring agents in the food and perfume industries. Synthetic monoterpene thiols have found an application in asymmetric synthesis as chiral auxiliaries, derivatizing agents, and ligands for metal complex catalysis and organocatalysts. Since monoterpenes and monoterpenoids are a renewable source, there are emerging trends to use monoterpene thiols as monomers for producing new types of green polymers. Monoterpene thioderivatives are also known to possess antioxidant, anticoagulant, antifungal, and antibacterial activity. The current review covers methods for the synthesis of acyclic, mono-, and bicyclic monoterpene thiols, as well as some investigations related to their usage for the preparation of the compounds with antimicrobial properties.

The spread of multidrug-resistant pathogenic microorganisms poses the challenge of searching for new antimicrobials with novel modes of action to which microorganisms have not yet developed resistance [19].The acquisition of genes encoding efflux systems or enzymes able to hydrolyze antimicrobials, the increased biofilm formation, and the structural changes in target molecules and the cell wall reduce the effectiveness of traditional antibiotics [20].
Among the various classes of molecules which can keep down the growth of pathogenic bacteria and fungi, monoterpene derivatives stand out for their broad spectrum of antimicrobial activity [21][22][23].The ability of monoterpenoids to inhibit the growth of diverse bacteria and fungi has been reported [21,[24][25][26][27][28][29].
The combination of terpenes with known antimicrobials increases the activity of the latter [30][31][32].The introduction of sulfur functional groups into the structure of biologically active terpenes often enhances the antibacterial and antifungal activity of the resulting thio-modified monoterpenoids compared to the original terpenes [21,29,[33][34][35][36]. Pinane and menthane sulfides containing a fragment of 2-mercaptoacetic acid methyl ester showed a wide range of antifungal activity against pathogenic strains of Candida albicans and a number of mycelial fungi [21,29].
The reason for these synergistic effects may be explained by the increased affinity of terpenes for the membrane or membrane-associated proteins.The binding site for cyclic hydrocarbons, including terpenes, is known to be in the cell membrane of pathogenic microorganisms [37].Some terpenes, such as limonene, αand β-pinenes, and γ-terpinene, can suppress respiration and other energy-dependent processes localized in the cell membranes of fungi and bacteria [22,[38][39][40][41]. Furthermore, some terpene derivatives interact with eukaryotic cell membranes [29,42].
Only a few reviews have been devoted to the synthesis and biological activity of thiomodified monoterpenoids [21,29,43].The current review covers methods for the synthesis of acyclic, mono-, and bicyclic monoterpene thiols, as well as some investigations related to their usage for preparing new compounds with antimicrobial properties.

Synthesis of Monoterpene Thiols
Thiols are one of the most convenient synthons in the synthesis of organosulfur compounds.The typical methods to prepare monoterpene thiols include the electrophilic addition of H 2 S or dithiols to the double bond of monoterpenes; nucleophilic substitution of halides; tosylates/mesylates obtained from corresponding monoterpene alcohols; thia-Michael addition of S-nucleophiles to α,β-unsaturated ketones; nucleophilic epoxide ring opening; nucleophilic substitution of the activated methylene protons; and reduction of sulfochlorides, dithiolanes, thiiranes, and sultones.

Synthesis from Alkenes
The synthesis of terpene thiols from limonene, α-pinene, α-, γ-terpinenes, terpinolene, and 3-carene via a reaction of them with H 2 S in the presence of Lewis acids such as AlCl 3 or AlBr 3 is described in [44].The addition of H 2 S usually occurs without selectivity and is accompanied by numerous side reactions, including the rearrangement of the terpene skeleton, especially in cases with bicyclic systems.The addition of H 2 S to limonene 1 catalyzed by AlCl 3 proceeds with no regioselectivity and gives thiols 2-5 in low yields, with the intramolecular cyclization of thiols 4 and 5 at the double bond affording sulfides 6 and 7 as the main products (Scheme 1) [45][46][47].
The combination of terpenes with known antimicrobials increases the activity of the la er [30][31][32].The introduction of sulfur functional groups into the structure of biologically active terpenes often enhances the antibacterial and antifungal activity of the resulting thio-modified monoterpenoids compared to the original terpenes [21,29,[33][34][35][36]. Pinane and menthane sulfides containing a fragment of 2-mercaptoacetic acid methyl ester showed a wide range of antifungal activity against pathogenic strains of Candida albicans and a number of mycelial fungi [21,29].
The reason for these synergistic effects may be explained by the increased affinity of terpenes for the membrane or membrane-associated proteins.The binding site for cyclic hydrocarbons, including terpenes, is known to be in the cell membrane of pathogenic microorganisms [37].Some terpenes, such as limonene, α-and β-pinenes, and γterpinene, can suppress respiration and other energy-dependent processes localized in the cell membranes of fungi and bacteria [22,[38][39][40][41]. Furthermore, some terpene derivatives interact with eukaryotic cell membranes [29,42].
Only a few reviews have been devoted to the synthesis and biological activity of thiomodified monoterpenoids [21,29,43].The current review covers methods for the synthesis of acyclic, mono-, and bicyclic monoterpene thiols, as well as some investigations related to their usage for preparing new compounds with antimicrobial properties.

Synthesis of Monoterpene Thiols
Thiols are one of the most convenient synthons in the synthesis of organosulfur compounds.The typical methods to prepare monoterpene thiols include the electrophilic addition of H2S or dithiols to the double bond of monoterpenes; nucleophilic substitution of halides; tosylates/mesylates obtained from corresponding monoterpene alcohols; thia-Michael addition of S-nucleophiles to α,β-unsaturated ketones; nucleophilic epoxide ring opening; nucleophilic substitution of the activated methylene protons; and reduction of sulfochlorides, dithiolanes, thiiranes, and sultones.

Synthesis from Alkenes
The synthesis of terpene thiols from limonene, α-pinene, α-, γ-terpinenes, terpinolene, and 3-carene via a reaction of them with H2S in the presence of Lewis acids such as AlCl3 or AlBr3 is described in [44].The addition of H2S usually occurs without selectivity and is accompanied by numerous side reactions, including the rearrangement of the terpene skeleton, especially in cases with bicyclic systems.The addition of H2S to limonene 1 catalyzed by AlCl3 proceeds with no regioselectivity and gives thiols 2-5 in low yields, with the intramolecular cyclization of thiols 4 and 5 at the double bond affording sulfides 6 and 7 as the main products (Scheme 1) [45][46][47].The interaction of α-pinene 8 with H2S under the same conditions leads to products 2-7, as well as cyclic sulfide 9 [44].The interaction of α-pinene 8 with H 2 S under the same conditions leads to products 2-7, as well as cyclic sulfide 9 [44].
The addition of hydrogen sulfide to 3-carene 14 in the presence of AlCl3 proceeds nonselectively to give the products in low yields.The detected products included a mixture of cis-and trans-thiols 15; episulfides 16, 6, and 7; and para-menthane thiols 17, 18, 2, and 3 (Scheme 3) [44].Reactions of racemic camphene 19 with thioacetic acid under various conditions were investigated in [48] (Scheme 4).It was established that, under catalyst-free conditions and with a long reaction time (12 h), the anti-Markovnikov product 20 was predominantly formed.The use of p-toluenesulfonic acid as a catalyst also leads to thioester 20, but in a 15% yield.Catalysis with trifluoromethanesulfonic acid (TfOH) and InCl3 at different temperatures gives different ratios of products.The optimal yield of thioacetate 21 (75%), a product of the Wagner-Meerwein rearrangement, was achieved using a catalyst TfOH at 40 °C for 20 min.The yield of a by-product, thioacetate 20, from this procedure does not exceed 25%.The best method to obtain Markovnikov product 22 (82%) with a preserving camphane structure was catalysis via In(OTf)3 at ≤0 °C.The deacylation of thioacetate 22 with LiAlH4 leads to racemic camphane thiol 23 at an 86% yield.The addition of hydrogen sulfide to 3-carene 14 in the presence of AlCl 3 proceeds nonselectively to give the products in low yields.The detected products included a mixture of cisand trans-thiols 15; episulfides 16, 6, and 7; and para-menthane thiols 17, 18, 2, and 3 (Scheme 3) [44].
The addition of hydrogen sulfide to 3-carene 14 in the presence of AlCl3 proceeds nonselectively to give the products in low yields.The detected products included a mixture of cis-and trans-thiols 15; episulfides 16, 6, and 7; and para-menthane thiols 17, 18, 2, and 3 (Scheme 3) [44].Reactions of racemic camphene 19 with thioacetic acid under various conditions were investigated in [48] (Scheme 4).It was established that, under catalyst-free conditions and with a long reaction time (12 h), the anti-Markovnikov product 20 was predominantly formed.The use of p-toluenesulfonic acid as a catalyst also leads to thioester 20, but in a 15% yield.Catalysis with trifluoromethanesulfonic acid (TfOH) and InCl3 at different temperatures gives different ratios of products.The optimal yield of thioacetate 21 (75%), a product of the Wagner-Meerwein rearrangement, was achieved using a catalyst TfOH at 40 °C for 20 min.The yield of a by-product, thioacetate 20, from this procedure does not exceed 25%.The best method to obtain Markovnikov product 22 (82%) with a preserving camphane structure was catalysis via In(OTf)3 at ≤0 °C.The deacylation of thioacetate 22 with LiAlH4 leads to racemic camphane thiol 23 at an 86% yield.Reactions of racemic camphene 19 with thioacetic acid under various conditions were investigated in [48] (Scheme 4).It was established that, under catalyst-free conditions and with a long reaction time (12 h), the anti-Markovnikov product 20 was predominantly formed.The use of p-toluenesulfonic acid as a catalyst also leads to thioester 20, but in a 15% yield.Catalysis with trifluoromethanesulfonic acid (TfOH) and InCl 3 at different temperatures gives different ratios of products.The optimal yield of thioacetate 21 (75%), a product of the Wagner-Meerwein rearrangement, was achieved using a catalyst TfOH at 40 • C for 20 min.The yield of a by-product, thioacetate 20, from this procedure does not exceed 25%.The best method to obtain Markovnikov product 22 (82%) with a preserving camphane structure was catalysis via In(OTf) 3 at ≤0 • C. The deacylation of thioacetate 22 with LiAlH 4 leads to racemic camphane thiol 23 at an 86% yield.
Photochemical addition of thioacetic acid to (−)-sabinene 24 gives a mixture of anti-Markovnikov bicyclic thioacetate 25 and unsaturated thioacetate 26 in an overall yield of 24% and a 3:1 ratio, respectively [49].The unexpected formation of thioacetate 26 results from cyclopropane ring cleavage.The mixture of thioacetates 25 and 26 was treated with LiAlH 4 to produce thiols 27 and 28 in an overall yield of 95% (Scheme 5).The obtained thiols were isolated by preparative capillary GC.Photochemical addition of thioacetic acid to (−)-sabinene 24 gives a mixture of anti Markovnikov bicyclic thioacetate 25 and unsaturated thioacetate 26 in an overall yield o 24% and a 3:1 ratio, respectively [49].The unexpected formation of thioacetate 26 result from cyclopropane ring cleavage.The mixture of thioacetates 25 and 26 was treated with LiAlH4 to produce thiols 27 and 28 in an overall yield of 95% (Scheme 5).The obtained thiols were isolated by preparative capillary GC.Scheme 5. Synthesis of thiols from sabinene 24.

Ene Reaction of Monoterpenes with N-sulfinylbenzenesulfonamide
An efficient method for the synthesis of monoterpene allyl thiols using N sulfinylbenzenesulfonamide 29 as an enophile in ene reaction was proposed in the pape [50] (Scheme 6).The interaction of terpenes (α-and β-pinenes 8 and 30; 2-and 3-carene 31 and 14; and α-thujene 32) with N-sulfinylbenzenesulfonamide 29 proceeds at a double bond with the formation of adducts 33-37 with a migration of the double bond to an α position.It should be noted that these reactions occur stereo-and regioselectively.The adducts 33-37, when reduced with LiAlH4, provide the corresponding allyl thiols, 38-42 Scheme 6. Synthesis of allylic terpene thiols 38-42.

Ene Reaction of Monoterpenes with N-sulfinylbenzenesulfonamide
An efficient method for the synthesis of monoterpene allyl thiols using N-sulfinyl benzenesulfonamide 29 as an enophile in ene reaction was proposed in the paper [50] (Scheme 6).The interaction of terpenes (α-and β-pinenes 8 and 30; 2-and 3-carenes 31 and 14; and α-thujene 32) with N-sulfinylbenzenesulfonamide 29 proceeds at a double bond with the formation of adducts 33-37 with a migration of the double bond to an α-position.It should be noted that these reactions occur stereo-and regioselectively.The adducts 33-37, when reduced with LiAlH 4 , provide the corresponding allyl thiols, 38-42.Photochemical addition of thioacetic acid to (−)-sabinene 24 gives a mixture of anti-Markovnikov bicyclic thioacetate 25 and unsaturated thioacetate 26 in an overall yield of 24% and a 3:1 ratio, respectively [49].The unexpected formation of thioacetate 26 results from cyclopropane ring cleavage.The mixture of thioacetates 25 and 26 was treated with LiAlH4 to produce thiols 27 and 28 in an overall yield of 95% (Scheme 5).The obtained thiols were isolated by preparative capillary GC.Scheme 5. Synthesis of thiols from sabinene 24.

Ene Reaction of Monoterpenes with N-sulfinylbenzenesulfonamide
An efficient method for the synthesis of monoterpene allyl thiols using Nsulfinylbenzenesulfonamide 29 as an enophile in ene reaction was proposed in the paper [50] (Scheme 6).The interaction of terpenes (α-and β-pinenes 8 and 30; 2-and 3-carenes 31 and 14; and α-thujene 32) with N-sulfinylbenzenesulfonamide 29 proceeds at a double bond with the formation of adducts 33-37 with a migration of the double bond to an αposition.It should be noted that these reactions occur stereo-and regioselectively.The adducts 33-37, when reduced with LiAlH4, provide the corresponding allyl thiols, 38-42.

Synthesis from α,β-Unsaturated Carbonyl Compounds
Thiols are good nucleophiles for thia-Michael addition to α,β-unsaturated carbonyl compounds [51].However, harsh reaction conditions are required to convert the newly formed sulfide group into a synthetically more versatile SH group.Thioacids (RCOSH) are more attractive as nucleophiles for the Michael addition reaction, since the resulting thioesters can be easily transformed into corresponding thiols under mild conditions [5,52,53].
Myrtenal-based hydroxythiol 43 was synthesized by two methods with a high yield and stereoselectivity [5].The treatment of (−)-myrtenal 44 with benzylthiol and 10% aqueous NaOH in THF at room temperature for 18 h led to sulfide 45 (yield 92%, de 96%).Compound 45 was reduced to the corresponding alcohol 46 (yield 96%) with LiAlH 4 in Et 2 O, which was then hydrogenolyzed to hydroxythiol 43 under Birch reduction conditions (Scheme 7).The hydrogenolysis did not provide satisfactory results because small differences in reaction conditions altered the reaction course dramatically, sometimes producing a complex mixture of unidentified compounds.The same reaction conditions become reproducible in switching to thioacetic acid as a nucleophilic reagent, which demonstrated a high selectivity when added to (−)-myrtenal 44 to give thioacetate 47 (1,4-addition) in yield of 98% and de > 99%.Thioester 47 was reduced by LiAlH 4 to obtain hydroxythiol 43 in a 95% yield.This one-pot method allowed us to simultaneously convert thioether and aldehyde group to the corresponding thiol and primary alcohol (Scheme 7).
Compound 45 was reduced to the corresponding alcohol 46 (yield 96%) with L Et2O, which was then hydrogenolyzed to hydroxythiol 43 under Birch re conditions (Scheme 7).The hydrogenolysis did not provide satisfactory results small differences in reaction conditions altered the reaction course dram sometimes producing a complex mixture of unidentified compounds.The same conditions become reproducible in switching to thioacetic acid as a nucleophilic which demonstrated a high selectivity when added to (−)-myrtenal 44 to give thi 47 (1,4-addition) in yield of 98% and de > 99%.Thioester 47 was reduced by L obtain hydroxythiol 43 in a 95% yield.This one-pot method allowed us to simulta convert thioether and aldehyde group to the corresponding thiol and primary (Scheme 7).Thioacetate 52 was obtained from (1S)-(−)-verbenone 53 by using a procedure similar to the synthesis of 2-formylisopinocampheyl-3-thioacetate 47.The reaction produces one of two theoretically possible diastereomers with the R-configuration of C-2 with a 71% yield (Scheme 8).Thioacetate 52 does not react with the Rupert-Prakash reagent under the above conditions, possibly because of the bulky TBAF use.yield (Scheme 8).Thioacetate 52 does not react with the Rupert-Prakash reagent unde the above conditions, possibly because of the bulky TBAF use.
The addition of fluorine-containing initiator CsF made it possible to obtain the only (4S)-diastereomer 54 in a 37% yield together with trifluoromethyl alcohol 55 (31%) that i a by-product of desulfurization (Scheme 8).Deacylation of thioacetate 54 gave hydroxythiol 56 in 73% yield [54].The synthesis of isomeric hydroxythiols 57-59 was carried out on the basis of β pinene 30 (Scheme 9) [55].Trans-pinocarveol 60 was synthesized via the oxidation of β pinene 30 with the SeO2/TBHP system, and its further oxidation with MnO2 led to pinocarvone 61.An inseparable mixture of two isomeric ketothioacetates (2S)-62 and (2R) 63 in a 2:1 ratio in 95% yield is formed during the thia-Michael reaction of pinocarvone 61 with AcSH in the presence of catalytic amount of pyridine at −5 °C.The reduction o thioacetates with LiAlH4 leads to three isomeric hydroxythiols, 57-59.The synthesis of pinane ketothiols 64 and 65 was implemented from α,β-unsaturated pinane ketones 61 and 66 [56].To obtain thioacetate 62 from enone 61, the synthetica protocol proposed in [5] was used.However, the diastereoselectivity of this reaction unde the described conditions did not exceed 33%, as mentioned in [55].The de value o thioacetate 62 can be increased from 33 up to 92% if the reaction between pinocarvone 61 and AcSH is carried out in THF in a temperature range from −60 to −65 °C, with pyridine as a co-solvent.The same conditions are applicable for the addition of BzSH to ketone 61 with thioacetate 67 being formed in this case with a comparable de of 93% (Scheme 10) Reducing thioacetate 62 via NH2NH2•H2O affords thiol 64 within 4-5 h in up to a 90% yield while deacylation of thiobenzoate 67 by the same reagent gives the thiol in only a 38-50% yield due to incomplete conversion.Thus, at comparable maximum de values of thioester 62 and 67, the preparation of thiol 64 from compound 62 is more optimal, taking into account the higher total yield of thiol and the diacylation time.The addition of fluorine-containing initiator CsF made it possible to obtain the only (4S)-diastereomer 54 in a 37% yield together with trifluoromethyl alcohol 55 (31%) that is a by-product of desulfurization (Scheme 8).Deacylation of thioacetate 54 gave hydroxythiol 56 in 73% yield [54].
The synthesis of isomeric hydroxythiols 57-59 was carried out on the basis of β-pinene 30 (Scheme 9) [55].Trans-pinocarveol 60 was synthesized via the oxidation of β-pinene 30 with the SeO 2 /TBHP system, and its further oxidation with MnO 2 led to pinocarvone 61.An inseparable mixture of two isomeric ketothioacetates (2S)-62 and (2R)-63 in a 2:1 ratio in 95% yield is formed during the thia-Michael reaction of pinocarvone 61 with AcSH in the presence of catalytic amount of pyridine at −5 • C. The reduction of thioacetates with LiAlH 4 leads to three isomeric hydroxythiols, 57-59.
Thioacetate 52 was obtained from (1S)-(−)-verbenone 53 by using a procedure similar to the synthesis of 2-formylisopinocampheyl-3-thioacetate 47.The reaction produces one of two theoretically possible diastereomers with the R-configuration of C-2 with a 71% yield (Scheme 8).Thioacetate 52 does not react with the Rupert-Prakash reagent under the above conditions, possibly because of the bulky TBAF use.
The addition of fluorine-containing initiator CsF made it possible to obtain the only (4S)-diastereomer 54 in a 37% yield together with trifluoromethyl alcohol 55 (31%) that is a by-product of desulfurization (Scheme 8).Deacylation of thioacetate 54 gave hydroxythiol 56 in 73% yield [54].The synthesis of pinane ketothiols 64 and 65 was implemented from α,β-unsaturated pinane ketones 61 and 66 [56].To obtain thioacetate 62 from enone 61, the synthetical protocol proposed in [5] was used.However, the diastereoselectivity of this reaction under the described conditions did not exceed 33%, as mentioned in [55].The de value of thioacetate 62 can be increased from 33 up to 92% if the reaction between pinocarvone 61 and AcSH is carried out in THF in a temperature range from −60 to −65 °C, with pyridine as a co-solvent.The same conditions are applicable for the addition of BzSH to ketone 61, with thioacetate 67 being formed in this case with a comparable de of 93% (Scheme 10).Reducing thioacetate 62 via NH2NH2•H2O affords thiol 64 within 4-5 h in up to a 90% yield, while deacylation of thiobenzoate 67 by the same reagent gives the thiol in only a 38-50% yield due to incomplete conversion.Thus, at comparable maximum de values of thioesters 62 and 67, the preparation of thiol 64 from compound 62 is more optimal, taking into account the higher total yield of thiol and the diacylation time.The synthesis of pinane ketothiols 64 and 65 was implemented from α,β-unsaturated pinane ketones 61 and 66 [56].To obtain thioacetate 62 from enone 61, the synthetical protocol proposed in [5] was used.However, the diastereoselectivity of this reaction under the described conditions did not exceed 33%, as mentioned in [55].The de value of thioacetate 62 can be increased from 33 up to 92% if the reaction between pinocarvone 61 and AcSH is carried out in THF in a temperature range from −60 to −65 • C, with pyridine as a co-solvent.The same conditions are applicable for the addition of BzSH to ketone 61, with thioacetate 67 being formed in this case with a comparable de of 93% (Scheme 10).Reducing thioacetate 62 via NH 2 NH 2 •H 2 O affords thiol 64 within 4-5 h in up to a 90% yield, while deacylation of thiobenzoate 67 by the same reagent gives the thiol in only a 38-50% yield due to incomplete conversion.Thus, at comparable maximum de values of thioesters 62 and 67, the preparation of thiol 64 from compound 62 is more optimal, taking into account the higher total yield of thiol and the diacylation time.A multistep synthesis of 2-norpinanone 66 from (−)-β-pinene 30 was provided in [57] (Scheme 11).This compound was obtained via nopinone 69 and then ketoenol 68 formation.Ketoenol 68 was produced in a 96% yield from ketone 69 by its reaction with isoamyl formate and t-BuOK in THF at 0 °C for 6 h [56].The following dihydroxylation of ketoalcohol 68 by formaldehyde in sodium carbonate solution afforded 2-norpinanone 66 [56].An addition of thioacetic acid to 2-norpinanone 66 was, for the first time, implemented according to the procedure [5] and then by using pyridine as a catalyst [51] in THF at room temperature [56].The main product of this reaction was the isomer (3R)-70 (de 98%) (Scheme 11).Its deacylation by hydrazine hydrate (NH2NH2•H2O) led to 2ketothiol 65 and disulfide 71 in a 3:1 ratio, respectively.Because of the mild reducing properties of NH2NH2•H2O and its inability to donate protons, the diacylation proceeds chemoselectively with the preservation of the carbonyl group [58], a behavior that is not typical for LiAlH4 when used [55].Isomeric α,β-hydroxythiols 77 and 78 were obtained from natural 3-carene 14 (Scheme 13) [63].3-Carene, when oxidized by m-CPBA, selectively forms trans-epoxide 79, which is isomerized in the presence of diethylaluminum 2,2,6-tetramethylpiperidide (DATMP) to enol 80 [64].The oxidation of alcohol 80 to enone 81 is successfully implemented by the bis(acetoxy)iodobenzene (BAIB)-2,2,6,6-tetramethylpiperidine 1oxyl (TEMPO) system.Enone 81, being an unstable compound, cannot be isolated in its A multistep synthesis of 2-norpinanone 66 from (−)-β-pinene 30 was provided in [57] (Scheme 11).This compound was obtained via nopinone 69 and then ketoenol 68 formation.Ketoenol 68 was produced in a 96% yield from ketone 69 by its reaction with isoamyl formate and t-BuOK in THF at 0 • C for 6 h [56].The following dihydroxylation of ketoalcohol 68 by formaldehyde in sodium carbonate solution afforded 2-norpinanone 66 [56].An addition of thioacetic acid to 2-norpinanone 66 was, for the first time, implemented according to the procedure [5] and then by using pyridine as a catalyst [51] in THF at room temperature [56].The main product of this reaction was the isomer (3R)-70 (de 98%) (Scheme 11).Its deacylation by hydrazine hydrate (NH 2 NH 2 •H 2 O) led to 2-ketothiol 65 and disulfide 71 in a 3:1 ratio, respectively.Because of the mild reducing properties of NH 2 NH 2 •H 2 O and its inability to donate protons, the diacylation proceeds chemoselec- tively with the preservation of the carbonyl group [58], a behavior that is not typical for LiAlH 4 when used [55].A multistep synthesis of 2-norpinanone 66 from (−)-β-pinene 30 was provided in [57] (Scheme 11).This compound was obtained via nopinone 69 and then ketoenol 68 formation.Ketoenol 68 was produced in a 96% yield from ketone 69 by its reaction with isoamyl formate and t-BuOK in THF at 0 °C for 6 h [56].The following dihydroxylation of ketoalcohol 68 by formaldehyde in sodium carbonate solution afforded 2-norpinanone 66 [56].An addition of thioacetic acid to 2-norpinanone 66 was, for the first time, implemented according to the procedure [5] and then by using pyridine as a catalyst [51] in THF at room temperature [56].The main product of this reaction was the isomer (3R)-70 (de 98%) (Scheme 11).Its deacylation by hydrazine hydrate (NH2NH2•H2O) led to 2ketothiol 65 and disulfide 71 in a 3:1 ratio, respectively.Because of the mild reducing properties of NH2NH2•H2O and its inability to donate protons, the diacylation proceeds chemoselectively with the preservation of the carbonyl group [58], a behavior that is not typical for LiAlH4 when used [55].Isomeric α,β-hydroxythiols 77 and 78 were obtained from natural 3-carene 14 (Scheme 13) [63].3-Carene, when oxidized by m-CPBA, selectively forms trans-epoxide 79, which is isomerized in the presence of diethylaluminum 2,2,6-tetramethylpiperidide (DATMP) to enol 80 [64].The oxidation of alcohol 80 to enone 81 is successfully implemented by the bis(acetoxy)iodobenzene (BAIB)-2,2,6,6-tetramethylpiperidine 1oxyl (TEMPO) system.Enone 81, being an unstable compound, cannot be isolated in its A multistep synthesis of 2-norpinanone 66 from (−)-β-pinene 30 was provided in [57] (Scheme 11).This compound was obtained via nopinone 69 and then ketoenol 68 formation.Ketoenol 68 was produced in a 96% yield from ketone 69 by its reaction with isoamyl formate and t-BuOK in THF at 0 °C for 6 h [56].The following dihydroxylation of ketoalcohol 68 by formaldehyde in sodium carbonate solution afforded 2-norpinanone 66 [56].An addition of thioacetic acid to 2-norpinanone 66 was, for the first time, implemented according to the procedure [5] and then by using pyridine as a catalyst [51] in THF at room temperature [56].The main product of this reaction was the isomer (3R)-70 (de 98%) (Scheme 11).Its deacylation by hydrazine hydrate (NH2NH2•H2O) led to 2ketothiol 65 and disulfide 71 in a 3:1 ratio, respectively.Because of the mild reducing properties of NH2NH2•H2O and its inability to donate protons, the diacylation proceeds chemoselectively with the preservation of the carbonyl group [58], a behavior that is not typical for LiAlH4 when used [55].Isomeric α,β-hydroxythiols 77 and 78 were obtained from natural 3-carene 14 (Scheme 13) [63].3-Carene, when oxidized by m-CPBA, selectively forms trans-epoxide 79, which is isomerized in the presence of diethylaluminum 2,2,6-tetramethylpiperidide (DATMP) to enol 80 [64].The oxidation of alcohol 80 to enone 81 is successfully implemented by the bis(acetoxy)iodobenzene (BAIB)-2,2,6,6-tetramethylpiperidine 1oxyl (TEMPO) system.Enone 81, being an unstable compound, cannot be isolated in its
pure form.The two-step thia-Michael addition of AcSH to α,β-unsaturated proceeds in one pot in pyridine.As a result, only one of the two theoretical diastereomers, thioacetate 82, is formed.The subsequent reduction of ketothi by LiAlH4 leads to two diastereomeric β-hydroxythiols, 77 and 78, in a respectively [63].
Int. J. Mol.Sci.2023, 24, x FOR PEER REVIEW 9 of 23 with zinc N,N-dimethyldithiocarbamate in the presence of triphenylphosphine and diethylazodicarboxylate (DEAD) is accompanied by an inversion of C-3 configuration and leads to dithiocarbamate 95 in a 66% yield.Dithiocarbamates baced on menthol 84 and borneol 89 were also obtained by the same procedure [73,74].The reduction of dithiocarbamate 95 by LiAlH4 gives thiol 93 in a 92% yield.The approach to obtain thiol 93 through the corresponding mesylate 96 and thioacetate 97 was described in [12].
Geraniol 98 reacts with thioacetic acid under Mitsunobu-type conditions [75] to form thioacetate 99 in a good yield, which, when treated with LiAlH4, is converted into the corresponding thiol 100 in a 61% yield (Scheme 16) [76].The ability of nerol 101 to be converted into bromide 102 under the action of PBr3, and then into thiol 103 by using NaSH via two successive nucleophilic substitutions with yields of 86 and 66%, respectively, was described in [77] (Scheme 17).
Int. J. Mol.Sci.2023, 24, x FOR PEER REVIEW 9 of 23 with zinc N,N-dimethyldithiocarbamate in the presence of triphenylphosphine and diethylazodicarboxylate (DEAD) is accompanied by an inversion of C-3 configuration and leads to dithiocarbamate 95 in a 66% yield.Dithiocarbamates baced on menthol 84 and borneol 89 were also obtained by the same procedure [73,74].The reduction of dithiocarbamate 95 by LiAlH4 gives thiol 93 in a 92% yield.The approach to obtain thiol 93 through the corresponding mesylate 96 and thioacetate 97 was described in [12].
Geraniol 98 reacts with thioacetic acid under Mitsunobu-type conditions [75] to form thioacetate 99 in a good yield, which, when treated with LiAlH4, is converted into the corresponding thiol 100 in a 61% yield (Scheme 16) [76].The ability of nerol 101 to be converted into bromide 102 under the action of PBr3, and then into thiol 103 by using NaSH via two successive nucleophilic substitutions with yields of 86 and 66%, respectively, was described in [77] (Scheme 17).

Scheme 17. Synthesis of thionerol 103.
Diastereomerically pure hydroxythiol 57 can also be obtained via two alternative routes [55].The first one involves the bromination of β-pinene 30 by NBS (Nbromosuccinimide) to form myrtenyl bromide 104, which undergoes hydroborationoxidation and is selectively transformed to bromoalcohol 105.The nucleophilic replacement of bromide by thioacetate AcS − leads to compound 106, which can also be synthesized starting from α-pinene 8 (Scheme 18).The second route is associated with the oxidation of α-pinene 8 to myrtenal, followed by its reduction to myrtenol 107, which is converted into diol 108 by the same hydroboration-oxidation procedure.The further reaction of tosyl chloride with diol 108 leads to both monotosylate 109 (76%) and ditosylate 110 (10%).The nucleophilic substitution of the para-toluenesulfonate group in 109 by AcS − also results in thioacetate 106.When reduced, thioacetate 106 affords hydroxythiol 57 (Scheme 18) [55].The ability of nerol 101 to be converted into bromide 102 under the action of PBr 3 , and then into thiol 103 by using NaSH via two successive nucleophilic substitutions with yields of 86 and 66%, respectively, was described in [77] (Scheme 17).
Int. J. Mol.Sci.2023, 24, x FOR PEER REVIEW 9 of 23 with zinc N,N-dimethyldithiocarbamate in the presence of triphenylphosphine and diethylazodicarboxylate (DEAD) is accompanied by an inversion of C-3 configuration and leads to dithiocarbamate 95 in a 66% yield.Dithiocarbamates baced on menthol 84 and borneol 89 were also obtained by the same procedure [73,74].The reduction of dithiocarbamate 95 by LiAlH4 gives thiol 93 in a 92% yield.The approach to obtain thiol 93 through the corresponding mesylate 96 and thioacetate 97 was described in [12].
Geraniol 98 reacts with thioacetic acid under Mitsunobu-type conditions [75] to form thioacetate 99 in a good yield, which, when treated with LiAlH4, is converted into the corresponding thiol 100 in a 61% yield (Scheme 16) [76].The ability of nerol 101 to be converted into bromide 102 under the action of PBr3, and then into thiol 103 by using NaSH via two successive nucleophilic substitutions with yields of 86 and 66%, respectively, was described in [77] (Scheme 17).

Scheme 17. Synthesis of thionerol 103.
Diastereomerically pure hydroxythiol 57 can also be obtained via two alternative routes [55].The first one involves the bromination of β-pinene 30 by NBS (Nbromosuccinimide) to form myrtenyl bromide 104, which undergoes hydroborationoxidation and is selectively transformed to bromoalcohol 105.The nucleophilic replacement of bromide by thioacetate AcS − leads to compound 106, which can also be synthesized starting from α-pinene 8 (Scheme 18).The second route is associated with the oxidation of α-pinene 8 to myrtenal, followed by its reduction to myrtenol 107, which is converted into diol 108 by the same hydroboration-oxidation procedure.The further reaction of tosyl chloride with diol 108 leads to both monotosylate 109 (76%) and ditosylate 110 (10%).The nucleophilic substitution of the para-toluenesulfonate group in 109 by AcS − also results in thioacetate 106.When reduced, thioacetate 106 affords hydroxythiol 57 (Scheme 18) [55].Diastereomerically pure hydroxythiol 57 can also be obtained via two alternative routes [55].The first one involves the bromination of β-pinene 30 by NBS (Nbromosuccinimide) to form myrtenyl bromide 104, which undergoes hydroboration-oxidation and is selectively transformed to bromoalcohol 105.The nucleophilic replacement of bromide by thioacetate AcS − leads to compound 106, which can also be synthesized starting from α-pinene 8 (Scheme 18).The second route is associated with the oxidation of α-pinene 8 to myrtenal, followed by its reduction to myrtenol 107, which is converted into diol 108 by the same hydroboration-oxidation procedure.The further reaction of tosyl chloride with diol 108 leads to both monotosylate 109 (76%) and ditosylate 110 (10%).The nucleophilic substitution of the para-toluenesulfonate group in 109 by AcS − also results in thioacetate 106.When reduced, thioacetate 106 affords hydroxythiol 57 (Scheme 18) [55].

Nucleophilic Substitution of the Activated Methylene Proton
The synthesis of bornane α-hydroxythiol 111 was described in [78,79]

Nucleophilic Substitution of the Activated Methylene Proton
The synthesis of bornane α-hydroxythiol 111 was described in [78,79]
Cis-epoxide 117 was obtained according to the known method [80] through bromohydrin 118 in 70% total yield.The interaction of epoxide 117 with AcSH in the presence of TMAF leads to thioacetate 119, the deacylation of which gives α-hydroxythiol 120 (Scheme 20) [63].

Nucleophilic Substitution of the Activated Methylene Proton
The synthesis of bornane α-hydroxythiol 111 was described in [78,79]
The nucleophilic sulfenylation of carane

Reduction of Thiiranes, Thiolanes, Sulfonyl Chlorides, and Sultones
Monoterpene thiols can be obtained via the reduction of thiiranes.A method for the directed synthesis of racemic thiol 4 from thiirane 131 through oxirane 132 and isothiouronium salt 133 was described in [47].The sequential reflux of epoxide 132 with thiourea and Na2CO3 leads to the corresponding thiirane 131, the reduction of which by LiAlH4 gives thiol 4 in a moderate yield.A similar protocol for obtaining racemic thiol 5 was reported in [1]; however, thiiran 134 in this study was synthesized from oxirane 135 using the N,N-dimethylthioformamide (DMTF)-TFA system as a reagent (Scheme 22).Trans-limonene-1,2-epoxide 137 and cis-1,2-limonene-1,2-epoxide 138 were transformed by the DMTF-TFA system into cis-139 and trans-1,2-epithio-p-ment-8-ene 140 respectively (Scheme 23) [2].The yield of thiirane 140 is lower than that of thiirane 139 since the reaction is accompanied by the formation of the by-product diol 141, which i yielded during the acid hydrolysis of epoxide 138.The reductive cleavage of the thiirane ring of 139 proceeds readily to give thiols 142 and 143, of which only thiol 142 was isolated in its pure form.Thiirane 140 was proposed to reduce to thiol 144 at only a 37% yield.

Reduction of Thiiranes, Thiolanes, Sulfonyl Chlorides, and Sultones
Monoterpene thiols can be obtained via the reduction of thiiranes.A method for the directed synthesis of racemic thiol 4 from thiirane 131 through oxirane 132 and isothiouronium salt 133 was described in [47].The sequential reflux of epoxide 132 with thiourea and Na 2 CO 3 leads to the corresponding thiirane 131, the reduction of which by LiAlH 4 gives thiol 4 in a moderate yield.A similar protocol for obtaining racemic thiol 5 was reported in [1]; however, thiiran 134 in this study was synthesized from oxirane 135 using the N,N-dimethylthioformamide (DMTF)-TFA system as a reagent (Scheme 22).yields.By-product disulfides 129 and 130 are additionally formed during the reacti thiiranes 121 and 122 with 2-mercaptoethanol (Scheme 21) [43].

Reduction of Thiiranes, Thiolanes, Sulfonyl Chlorides, and Sultones
Monoterpene thiols can be obtained via the reduction of thiiranes.A method fo directed synthesis of racemic thiol 4 from thiirane 131 through oxirane 132 isothiouronium salt 133 was described in [47].The sequential reflux of epoxide 132 thiourea and Na2CO3 leads to the corresponding thiirane 131, the reduction of whic LiAlH4 gives thiol 4 in a moderate yield.A similar protocol for obtaining racemic th was reported in [1]; however, thiiran 134 in this study was synthesized from oxiran using the N,N-dimethylthioformamide (DMTF)-TFA system as a reagent (Scheme 22 Trans-limonene-1,2-epoxide 137 and cis-1,2-limonene-1,2-epoxide 138 transformed by the DMTF-TFA system into cis-139 and trans-1,2-epithio-p-ment-8-ene respectively (Scheme 23) [2].The yield of thiirane 140 is lower than that of thiirane since the reaction is accompanied by the formation of the by-product diol 141, whi yielded during the acid hydrolysis of epoxide 138.The reductive cleavage of the thi ring of 139 proceeds readily to give thiols 142 and 143, of which only thiol 142 was iso in its pure form.Thiirane 140 was proposed to reduce to thiol 144 at only a 37% yield Scheme 22. Scheme for the synthesis of racemic 1-p-menthene-8-thiol 4 and 1-p-menthene-4-thiol 5.
Trans-limonene-1,2-epoxide 137 and cis-1,2-limonene-1,2-epoxide 138 were transformed by the DMTF-TFA system into cis-139 and trans-1,2-epithio-p-ment-8-ene 140, respectively (Scheme 23) [2].The yield of thiirane 140 is lower than that of thiirane 139, since the reaction is accompanied by the formation of the by-product diol 141, which is yielded during the acid hydrolysis of epoxide 138.The reductive cleavage of the thiirane ring of 139 proceeds readily to give thiols 142 and 143, of which only thiol 142 was isolated in its pure form.Thiirane 140 was proposed to reduce to thiol 144 at only a 37% yield.Scheme 26.Reduction of monoterpene sultones 154 and 155.
The antimicrobial activity of the newly synthesized sulfenimines 166a-f, 167a-f, and Compounds 161a, (S S )-162b, (R S S)-164a, (S S R)-164b, (R S R)-165a, and (S S S)-165b at a concentration of 32 µg/mL showed antibacterial activity against Acinetobacter baumannii, and sulfinamide (R S R)-165a has antifungal activity against Candida albicans.The MIC (minimum inhibitory concentration) value of (R S R)-165a against Candida was 0.25 µg/mL.This compound also showed moderate cytotoxicity against human embryonic kidney cells (Hek-293) at a concentration of 32 µg/mL.All of this indicates that sulfinamide (R S R)-165a is not only a selective antifungal agent but also a promising compound for further medical trials.
Unsymmetrical disulfides 169a-d with a neomentane fragment showed antimicrobial activity against both S. aureus strains, with MICs of 16-32 µg/mL.Disulfides 170b (MIC 16 µg/mL) and 170d (MIC 16 µg/mL) have the highest activity against the MSSA among the compounds 170a-d.Disulfides 172a-c bearing an OH group at the C-3 position of the terpene fragment did not demonstrate any antibacterial properties.Pinane disulfides 171a-c with a hydroxymethyl group at C-10 in their biological activity turned out to be similar to neomentane thiotherpenoids 169a-c and showed MIC values of 32-64 µg/mL.Only disulfides 169a-c, 170a, 170b, and 171a were capable of inhibiting Pseudomonas aeruginosa.Along with that, there were no disulfides among (169-172)a-c with pronounced antifungal activity against the clinical isolate of C. albicans.However, disulfides 169-172d containing a 2-mercaptonicotinic acid moiety nevertheless demonstrated antifungal activity (MIC 16-128 µg/mL).
In general, the synthesized asymmetric monoterpenyl hetaryl disulfides (169-172)ad possess high cytotoxicity (CC50) against EBL.Pinane disulfides 170a, 170b, and 171d showed the lowest toxicity.For neomenthane disulfides 169a and 169b, mutagenicity was revealed in the Ames test on Salmonella typhimurium [97].The antimicrobial activity of the newly synthesized sulfenimines 166a-f, 167a-f, and 168a was assessed against Gram-positive methicillin-susceptible S. aureus (MSSA) and methicillin-resistant S. aureus (MRSA), Gram-negative bacterium P. aeruginosa, and a fluconazole-sensitive C. albicans.These microorganisms are characterized by a high frequency of resistant isolates and cause diseases of various mucous membranes, the skin, and the respiratory tract.
Compounds 166a, 167a, 166b, and 167e inhibited the growth of all tested pathogens, although the activity was moderate and the MIC values (8-64 µg/mL) were generally higher than those of the reference antimicrobials (amikacin, ampicillin, ciprofloxacin, fluconazole, and benzalkonium chloride).It is important to note that trifluoromethylated sulfenimines with salicylic fragments 168a and 167f were active only against methicillin-resistant S. aureus and C. albicans, and 168a was even more active than fluconazole (MIC 8 µg/mL).In addition, sulfenimines with a CF 3 group in the terpene moiety and salicylaldehyde fragment 167a, 168a, 167b, and 167f exhibit greater antifungal activity (MIC 8-32 µg/mL) in contrast to the non-fluorinated analogues 166a, 166e, and 166f (MIC ≥ 64 µg/mL).
However, most of the synthesized compounds are highly cytotoxic to embryonic bovine lung (EBL) cells.All new compounds have selectivity indices (SI, the ratio of toxicity to MIC) of 2-4, showing their high relative toxicity, which reduces the possibility to further use these compounds as potential antibiotics and indicates the need for further optimization of the structure with reducing the negative effect on eukaryotic cells.
In general, the synthesized asymmetric monoterpenyl hetaryl disulfides (169-172)ad possess high cytotoxicity (CC50) against EBL.Pinane disulfides 170a, 170b, and 171d showed the lowest toxicity.For neomenthane disulfides 169a and 169b, mutagenicity was revealed in the Ames test on Salmonella typhimurium [97].Unsymmetrical disulfides 169a-d with a neomentane fragment showed antimicrobial activity against both S. aureus strains, with MICs of 16-32 µg/mL.Disulfides 170b (MIC 16 µg/mL) and 170d (MIC 16 µg/mL) have the highest activity against the MSSA among the compounds 170a-d.Disulfides 172a-c bearing an OH group at the C-3 position of the terpene fragment did not demonstrate any antibacterial properties.Pinane disulfides 171a-c with a hydroxymethyl group at C-10 in their biological activity turned out to be similar to neomentane thiotherpenoids 169a-c and showed MIC values of 32-64 µg/mL.Only disulfides 169a-c, 170a, 170b, and 171a were capable of inhibiting Pseudomonas aeruginosa.Along with that, there were no disulfides among (169-172)a-c with pronounced antifungal activity against the clinical isolate of C. albicans.However, disulfides 169-172d containing a 2-mercaptonicotinic acid moiety nevertheless demonstrated antifungal activity (MIC 16-128 µg/mL).

Application of Monoterpene Thiols in Asymmetric Synthesis
Monoterpene thiols, known for their natural enantiomeric purity, have found applications in asymmetric synthesis.To reveal the synthetic potential of monoterpene thiols, we provide some examples of their application in asymmetric synthesis.
As an example, the work of [5] can be given, which covers a method of using pinane hydroxythiol 43 as a chiral auxiliary to synthesize certain chiral aldols and diols (Scheme 32).When thiol 43 was treated with α,α-dimethoxyacetone, a single diastereomer, ketooxathiane 182, was formed with a yield of 32%.The further addition of Grignard reagents and organolithium compounds at the C=O of 182 afforded the corresponding alcohols 183a-g in good yields and high diastereoselectivity.The configuration of a newly formed chiral center of the major diastereomers was assigned as R for tertiary alcohols 183a-f and S for a secondary one, 183g, due to the change in seniority of substituents.LS-Selectride (lithium trisiamylborohydride) reduces ketone 182 more selectively than LiAlH 4 and DIBAL (diisobutylaluminum hydride).Compounds 183a-g reacted with AgNO 3 and NCS by opening the oxothiane ring to give sultine 184 and aldols 185a-g, which are not isolated in an individual form.By reducing with LiAlH 4 , this mixture was converted into the separable non-racemic thiol 43 (63-72%) and diols 186a-g in a yield of 74 up to 83%.
LiAlH4 and DIBAL (diisobutylaluminum hydride).Compounds 183a-g reacted with AgNO3 and NCS by opening the oxothiane ring to give sultine 184 and aldols 185a-g, which are not isolated in an individual form.By reducing with LiAlH4, this mixture was converted into the separable non-racemic thiol 43 (63-72%) and diols 186a-g in a yield of 74 up to 83%.
The similar approaches using hydroxythiol 43 for the preparation of chiral diols, as well as α-hydroxy acids, are also described in [99][100][101].
Chiral bornane 1,2-and 1,3-hydroxythiols 111, 150, and 151 were evaluated as catalysts for the asymmetric reduction of prochiral ketones with borane (Scheme 33) [14,15].Thus, acetophenone 187 was reduced to 1-phenylethanol in yields greater than 90% and in good enantioselectivity.The solvent nature did not affect the reaction enantioselectivity, and the stoichiometric ratio of catalyst to substrate used slightly increased it to 75%.In another work [102], a 96% yield and 87% ee were achieved for alcohol 188 by replacing the boron hydrogenating agent with borane dimethyl sulfide, conducting the reaction in toluene at 50 °C with hydroxythiol 111 as an organocatalyst.
The similar approaches using hydroxythiol 43 for the preparation of chiral diols, as well as α-hydroxy acids, are also described in [99][100][101].
Chiral bornane 1,2-and 1,3-hydroxythiols 111, 150, and 151 were evaluated as catalysts for the asymmetric reduction of prochiral ketones with borane (Scheme 33) [14,15].Thus, acetophenone 187 was reduced to 1-phenylethanol in yields greater than 90% and in good enantioselectivity.The solvent nature did not affect the reaction enantioselectivity, and the stoichiometric ratio of catalyst to substrate used slightly increased it to 75%.In another work [102], a 96% yield and 87% ee were achieved for alcohol 188 by replacing the boron hydrogenating agent with borane dimethyl sulfide, conducting the reaction in toluene at 50 • C with hydroxythiol 111 as an organocatalyst.

Conclusions
In summary, the synthesis of acyclic, mono-, and bicyclic monoterpene thiols has been achieved via numerous pathways.The current review outlines a wide range of reactions to demonstrate the synthetic importance of functionalized monoterpenoids.In addition to focusing on the synthesis of monoterpene thiols, this review also examines their use as convenient and versatile synthons in organic synthesis and for the production of bioactive compounds.

Conclusions
In summary, the synthesis of acyclic, mono-, and bicyclic monoterpene thiols has been achieved via numerous pathways.The current review outlines a wide range of reactions to demonstrate the synthetic importance of functionalized monoterpenoids.In addition to focusing on the synthesis of monoterpene thiols, this review also examines their use as convenient and versatile synthons in organic synthesis and for the production of bioactive compounds.

Scheme 1 .
Scheme 1.The addition of H 2 S to limonene 1 catalyzed by AlCl 3 .
cover the methods for the selective preparation of neomenthanethiol 83 using thioacetic acid (AcSH) (Scheme 14).Starting menthol 84 reacts with p-TsCl in pyridine to form tosylate 85, which, when heated with AcSK, gives thioacetate 86 in a 77% yield.Substitution of the OTs (p-toluenesulfonate, tosylate) by the AcS-group occurs with an inversion of the chiral center via the SN2 mechanism.The reduction of 86 by LiAlH4 provides diastereomerically pure thiol 83 in a 26-40% yield (Scheme 14).
cover the methods for the selective prep neomenthanethiol 83 using thioacetic acid (AcSH) (Scheme 14).Starting menth with p-TsCl in pyridine to form tosylate 85, which, when heated with A thioacetate 86 in a 77% yield.Substitution of the OTs (p-toluenesulfonate, tosy AcS-group occurs with an inversion of the chiral center via the SN2 mech reduction of 86 by LiAlH4 provides diastereomerically pure thiol 83 in a 26 (Scheme 14).
(Scheme 19).The nucleophilic substitution of a proton of the activated methylene group in camphor 112 by benzyl p-toluenesulfonate promoted by LDA leads to the formation of ketosulfide 113, which, being reduced by NaBH4 in methanol or dibutylaluminum hydride (DIBAL) in THF, gives hydroxysulfide 114, which is capable of being transformed into hydroxythiol 111 by the Birch reduction.
(Scheme 19).The nucleophilic substitution of a proton of the activated methylene group in camphor 112 by benzyl p-toluenesulfonate promoted by LDA leads to the formation of ketosulfide 113, which, being reduced by NaBH 4 in methanol or dibutylaluminum hydride (DIBAL) in THF, gives hydroxysulfide 114, which is capable of being transformed into hydroxythiol 111 by the Birch reduction.
(Scheme 19).The nucleophilic substitution of a proton of the activated methylene group in camphor 112 by benzyl p-toluenesulfonate promoted by LDA leads to the formation of ketosulfide 113, which, being reduced by NaBH4 in methanol or dibutylaluminum hydride (DIBAL) in THF, gives hydroxysulfide 114, which is capable of being transformed into hydroxythiol 111 by the Birch reduction.
(Scheme 19).The nucleophilic substitution of a proton of the activated methylene group in camphor 112 by benzyl p-toluenesulfonate promoted by LDA leads to the formation of ketosulfide 113, which, being reduced by NaBH4 in methanol or dibutylaluminum hydride (DIBAL) in THF, gives hydroxysulfide 114, which is capable of being transformed into hydroxythiol 111 by the Birch reduction.