Biocatalytic Thionation of Epoxides for Enantioselective Synthesis of Thiiranes

Ma, Ran; Hua, Xia; He, Cheng-Li; Wang, Zhu-Xiang; Cui, Bao‐Dong; Han, Wen‐Yong; Chen, Yong‐Zheng; Wan, Nan‐Wei

doi:10.1002/anie.202212589

Cited by 11 publications

(11 citation statements)

References 76 publications

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“…In the reverse epoxide ring-opening reaction, the enzyme can take other nucleophiles, such as azide, cyanide, nitrite, cyanate, or thiocyanate, to form new C−N, C−O, C− C, and C−S bonds. 33,34 In recent years, based on the two specific sequence motifs "T-X 4 -F/Y-X-G" and "S-X 12 -Y-X 3 -R", which were derived from multiple sequence alignments of the known HHDHs, a large number of haloalcohol dehalogenases have been discovered and divided into A−G subgroups. 35 ArHheC, one of the subfamily C HHDHs, showed good βattack preference and stereoselectivity in the ring opening of alkyl epoxide using cyanate as a nucleophile to produce 5substituted oxazolidinones, 36 while low stereoselectivity and regioselectivity were observed when styrene oxide was used as the substrate (34:66 α/β) (Scheme 1e).…”

Section: ■ Introductionmentioning

confidence: 99%

“…4.5.1.-) catalyze the reversible dehalogenation of α-halo alcohols to form epoxides. In the reverse epoxide ring-opening reaction, the enzyme can take other nucleophiles, such as azide, cyanide, nitrite, cyanate, or thiocyanate, to form new C–N, C–O, C–C, and C–S bonds. , In recent years, based on the two specific sequence motifs “T-X 4 -F/Y-X-G” and “S-X 12 -Y-X 3 -R”, which were derived from multiple sequence alignments of the known HHDHs, a large number of haloalcohol dehalogenases have been discovered and divided into A–G subgroups while low stereoselectivity and regioselectivity were observed when styrene oxide was used as the substrate (34:66 α/β) (Scheme e) .…”

Section: Introductionmentioning

confidence: 99%

“…The extremely low reaction temperature and the formation of different binding conformations of nucleophile nitrite in the halide-binding site were the main reasons for the success of the reaction. When thiocyanate was used as the nucleophile in the ring opening of epoxides catalyzed by HHDHapb 34 and its mutant M4, chiral thiiranes were obtained with high ee by the enzymatic ring opening of epoxides and a subsequent non-enzymatic rearrangement. The isolation of reaction intermediates revealed that thiocyanate could attack either the C α or C β of epoxides.…”

Section: ■ Introductionmentioning

confidence: 99%

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Flipping the Substrate Creates a Highly Selective Halohydrin Dehalogenase for the Synthesis of Chiral 4-Aryl-2-oxazolidinones from Readily Available Epoxides

Zhou

Chen

et al. 2023

ACS Catal.

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Chiral oxazolidinones are a class of important heterocyclic compounds in pharmaceutical chemistry due to their biological activity. Halohydrin dehalogenase-catalyzed epoxide ring-opening reaction with cyanate offers an attractive approach to the synthesis of chiral oxazolidinones, but the α/β-regioselectivity and stereoselectivity are still un-addressed issues. In this study, a unique halohydrin dehalogenase (AbHheG) was found to have high activity and α/β-regioselectivity toward the ring opening of racemic styrene oxide with cyanate but with poor stereoselectivity (E < 3). By reshaping the substrate-binding site of AbHheG, a variant Y15M/N182S was obtained with excellent α/β-regioselectivity and stereoselectivity. The variant showed E > 200 for 9 of the 13 tested styrene oxides. Since (R)-4-aryl-2-oxazolidinones were easily separated from (R)-styrene oxides, both (R)- and (S)-4-aryl-2-oxazolidinones could be readily prepared. Crystallographic and enzyme–substrate docking analysis showed that flipping of the substrate in the binding site resulted in the R-configuration substrate being away from the catalytic triad in the mutant, which was responsible for the enhanced α/β-regioselectivity and stereoselectivity. This work has demonstrated that halohydrin dehalogenase is a useful biocatalyst for the synthesis of both enantiomers of 4-aryl-2-oxazolidinones from readily available racemic styrene oxides. The structural and computational studies provide a guidance for further engineering of halohydrin dehalogenases to control the α/β-regioselectivity and stereoselectivity for the efficient synthesis of the desired optically pure 4- or 5-substituted 2-oxazolidinones.

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Section: ■ Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: ■ Introductionmentioning

confidence: 99%

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Flipping the Substrate Creates a Highly Selective Halohydrin Dehalogenase for the Synthesis of Chiral 4-Aryl-2-oxazolidinones from Readily Available Epoxides

Zhou

Chen

et al. 2023

ACS Catal.

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“…HHDHs can catalyze not only the formation of epoxides through dehalogenation of vicinal halohydrins but also the generation of β-substituted alcohols or its derivatives through the ring-opening of epoxides in the presence of several anionic nucleophiles, such as cyanide, azide, cyanate, nitrite, and thiocyanate (Figure S1). , Many HHDHs have been identified and engineered for the synthesis of various chiral compounds, such as epoxides, − β-halohydrins, − β-hydroxy nitriles, − β-azidoalcohols, − oxazolidinones, − β-nitroalcohols, and thiiranes . In particular, chiral β-hydroxy nitriles are a ubiquitous class of cyano-containing compounds present in many pharmaceuticals (Scheme a). − For instance, the chiral β-hydroxy nitrile moiety is a crucial component of remdesivir (GS-5734), which is a nucleoside analogue with potent antiviral activity .…”

Section: Introductionmentioning

confidence: 99%

Biocatalytic Enantioselective Synthesis of Chiral β-Hydroxy Nitriles Using Cyanohydrins as Cyano Sources

Guan,

Miao,

Hua

et al. 2023

ACS Catal.

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The development of catalytic enantioselective cyanation methods for preparing valuable chiral nitriles is of great interest in the areas of pharmaceutical synthesis and organic chemistry. In this study, we presented an enzymatic enantioselective cyanation strategy for the synthesis of chiral β-hydroxy nitriles using cyanohydrins as cyano sources. By combining enzyme screening and protein engineering of halohydrin dehalogenases, biocatalytic enantioselective cyanation of various aryl, alkyl, and spiro epoxides was achieved to afford the corresponding chiral β-hydroxy nitriles in good yields (up to 47%) and excellent optical purities (up to >99% ee). Additionally, we also demonstrated that the biocatalytic cyanation method can be used for the enantiocomplementary and large-scale synthesis of chiral β-hydroxy nitriles.

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“…Halohydrin dehalogenases (HHDHs) have the ability to catalyze the dehalogenation of vicinal halohydrins to epoxides, releasing protons and halide ions in the process . In addition, HHDHs can also catalyze ring-opening reactions of epoxides in the presence of several anionic nucleophiles, such as cyanide, nitrite, azide, thiocyanate, and cyanate, resulting in the generation of β-substituted alcohols or their derivatives. In particular, the enzymatic ring-opening reaction of epoxides with cyanate (OCN – ) generates unstable isocyanates and cyanate adducts, which can be easily converted to oxazolidinones by undergoing a spontaneous cyclization reaction .…”

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confidence: 99%

Biocatalytic Synthesis of Metaxalone and Its Analogues

Wang,

Fu,

et al. 2023

Org. Lett.

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A biocatalytic approach for the synthesis of metaxalone and its analogues was developed based on the reaction of epoxides and cyanate catalyzed by halohydrin dehalogenase. Gram-scale synthesis of chiral and racemic metaxalone was achieved with 44% (98% ee) and 81% yields, respectively, by protein engineering of the halohydrin dehalogenase HHDHamb from Acidimicrobiia bacterium. Additionally, various metaxalone analogues were synthesized at 28–40% yields (90–99% ee) for chiral forms and 77–92% yields for racemic forms.

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Biocatalytic Thionation of Epoxides for Enantioselective Synthesis of Thiiranes

Cited by 11 publications

References 76 publications

Flipping the Substrate Creates a Highly Selective Halohydrin Dehalogenase for the Synthesis of Chiral 4-Aryl-2-oxazolidinones from Readily Available Epoxides

Flipping the Substrate Creates a Highly Selective Halohydrin Dehalogenase for the Synthesis of Chiral 4-Aryl-2-oxazolidinones from Readily Available Epoxides

Biocatalytic Enantioselective Synthesis of Chiral β-Hydroxy Nitriles Using Cyanohydrins as Cyano Sources

Biocatalytic Synthesis of Metaxalone and Its Analogues

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