A Biocatalytic Platform for Synthesis of Chiral α-Trifluoromethylated Organoborons
Abstract
There are few biocatalytic transformations that produce fluorine-containing molecules prevalent in modern pharmaceuticals. To expand the scope of biocatalysis for organofluorine synthesis, we have developed an enzymatic platform for highly enantioselective carbene B–H bond insertion to yield versatile α-trifluoromethylated (α-CF_3) organoborons, an important class of organofluorine molecules that contain stereogenic centers bearing both CF_3 and boron groups. In contrast to current "carbene transferase" enzymes that use a limited set of simple diazo compounds as carbene precursors, this system based on Rhodothermus marinus cytochrome c (Rma cyt c) can accept a broad range of trifluorodiazo alkanes and deliver versatile chiral α-CF_3 organoborons with total turnovers up to 2870 and enantiomeric ratios up to 98.5:1.5. Computational modeling reveals that this broad diazo scope is enabled by an active-site environment that directs the alkyl substituent on the heme CF_3-carbene intermediate toward the solvent-exposed face, thereby allowing the protein to accommodate diazo compounds with diverse structural features.
Additional Information
© 2019 American Chemical Society. ACS AuthorChoice - This is an open access article published under an ACS AuthorChoice License, which permits copying and redistribution of the article or any adaptations for non-commercial purposes. Received: September 25, 2018; Published: February 1, 2019. We thank Kai Chen, Zhijun Jia, and Russell Lewis for helpful discussions. This work was supported by National Institutes of Health, National Institute for General Medical Sciences, GM-124480 (to K.N.H.); Jacobs Institute for Molecular Engineering for Medicine at Caltech (F.H.A.); National Science Foundation Division of Molecular and Cellular Biosciences Grant MCB-1513007 (F.H.A.). X.H. is supported by an NIH pathway to independence award (Grant K99GM129419). M.G.-B. thanks the Ramón Areces Foundation for a postdoctoral fellowship. Computational resources were provided by the University of California, Los Angeles Institute for Digital Research and Education and the Extreme Science and Engineering Discovery Environment, which is supported by National Science Foundation Grant OCI-1053575. Author Contributions: X.H. and M.G.-B. contributed equally to this work. The authors declare no competing financial interest.Attached Files
Published - acscentsci.8b00679.pdf
Submitted - 180925-CF3_Organoborons.pdf
Supplemental Material - oc8b00679_si_001.pdf
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Additional details
- PMCID
- PMC6396380
- Eprint ID
- 90359
- Resolver ID
- CaltechAUTHORS:20181023-102546587
- GM-124480
- NIH
- Jacobs Institute for Molecular Engineering for Medicine
- MCB-1513007
- NSF
- K99GM129419
- NIH
- Ramón Areces Foundation
- OCI-1053575
- NSF
- Created
-
2018-10-23Created from EPrint's datestamp field
- Updated
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2022-03-01Created from EPrint's last_modified field
- Caltech groups
- Jacobs Institute for Molecular Engineering for Medicine