{Reference Type}: Journal Article
{Title}: Discovery, characterization and mechanism of a Microbacterium esterase for key d-biotin chiral intermediate synthesis.
{Author}: Li X;Yu H;Liu S;Ma B;Wu X;Zheng X;Xu Y;
{Journal}: Bioresour Bioprocess
{Volume}: 11
{Issue}: 1
{Year}: 2024 Jun 16
{Factor}: 4.983
{DOI}: 10.1186/s40643-024-00776-2
{Abstract}: Esterases are crucial biocatalysts in chiral compound synthesis. Herein, a novel esterase EstSIT01 belonging to family V was identified from Microbacterium chocolatum SIT101 through genome mining and phylogenetic analysis. EstSIT01 demonstrated remarkable efficiency in asymmetrically hydrolyzing meso-dimethyl ester [Dimethyl cis-1,3-Dibenzyl-2-imidazolidine-4,5-dicarboxyate], producing over 99% yield and 99% enantiomeric excess (e.e.) for (4S, 5R)-monomethyl ester, a crucial chiral intermediate during the synthesis of d-biotin. Notably, the recombinant E. coli expressing EstSIT01 exhibited over 40-fold higher activity than that of the wild strain. EstSIT01 displays a preference for short-chain p-NP esters. The optimal temperature and pH were 45 °C and 10.0, with Km and kcat values of 0.147 mmol/L and 5.808 s- 1, respectively. Molecular docking and MD simulations suggest that the high stereoselectivity for meso-diester may attribute to the narrow entrance tunnel and unique binding pocket structure. Collectively, EstSIT01 holds great potential for preparing chiral carboxylic acids and esters.