脱氧胆酸
化学
生物催化
羟基化
血红素
组合化学
细胞色素P450
催化作用
立体选择性
生物化学
立体化学
酶
胆汁酸
反应机理
作者
Chixiang Sun,Baodong Hu,Yanchun Li,Zhimeng Wu,Jingwen Zhou,Jianghua Li,Jian Chen,Guocheng Du,Xinrui Zhao
标识
DOI:10.1016/j.synbio.2023.11.008
摘要
Deoxycholic acid (DCA) has been authorized by the Federal Drug Agency for cosmetic reduction of redundant submental fat. The hydroxylated product (6β-OH DCA) was developed to improve the solubility and pharmaceutic properties of DCA for further applications. Herein, a combinatorial catalytic strategy was applied to construct a powerful Cytochrome P450 biocatalyst (CYP107D1, OleP) to convert DCA to 6β-OH DCA. Firstly, the weak expression of OleP was significantly improved using pRSFDuet-1 plasmid in the E. coli C41 (DE3) strain. Next, the supply of heme was enhanced by the moderate overexpression of crucial genes in the heme biosynthetic pathway. In addition, a new biosensor was developed to select the appropriate redox partner. Furthermore, a cost-effective whole-cell catalytic system was constructed, resulting in the highest reported conversion rate of 6β-OH DCA (from 4.8% to 99.1%). The combinatorial catalytic strategies applied in this study provide an efficient method to synthesize high-value-added hydroxylated compounds by P450s.
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