Preparative access to medicinal chemistry related chiral alcohols using carbonyl reductase technology
Libraries of highly enantioenriched secondary alcohols in both enantiomeric forms were synthesized by enzymatic reduction of their parent ketones using selectAZyme™ carbonyl reductase (CRED) technology.
Commercially available CREDs were able to reduce a range of substrate classes efficiently and with very high enantioselectivity. Matching substrate classes to small subsets of CREDs enabled the fast development of preparative bioreductions and the rapid generation of 100–1500 mg samples of chiral alcohols in typically >95% ee and the majority in P99.0% ee.
The conditions for small scale synthesis were then scaled up to 0.5 kg to deliver one of the chiral alcohols, (S)-1-(4-bromophenyl)-2-chloroethanol, in 99.8% ee and 91% isolated yield.
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