Characterization of a Carbonyl Reductase from WZ010 and Its Variant Y54F for Asymmetric Synthesis of ()--Boc-3-Hydroxypiperidine.

The recombinant carbonyl reductase from WZ010 (ReCR) demonstrated strict ()-stereoselectivity and catalyzed the irreversible reduction of -Boc-3-piperidone (NBPO) to ()--Boc-3-hydroxypiperidine [()-NBHP], a key chiral intermediate in the synthesis of ibrutinib. The NAD(H)-specific enzyme was active within broad ranges of pH and temperature and had remarkable activity in the presence of higher concentration of organic solvents. The amino acid residue at position 54 was critical for the activity and the substitution of Tyr54 to Phe significantly enhanced the catalytic efficiency of ReCR. The / values of ReCR Y54F for NBPO, (/)-2-octanol, and 2-propanol were 49.17 s mM, 56.56 s mM, and 20.69 s mM, respectively. In addition, the ()-NBHP yield was as high as 95.92% when whole cells of overexpressing ReCR variant Y54F catalyzed the asymmetric reduction of 1.5 M NBPO for 12 h in the aqueous/(/)-2-octanol biphasic system, demonstrating the great potential of ReCR variant Y54F for practical applications.