Docking-guided rational engineering of a macrolide glycosyltransferase glycodiversifies epothilone B

Author:

Zhang Peng,Zhang Lijuan,Jiang XukaiORCID,Diao Xiao-tong,Li Shuang,Li Dan-dan,Zhang Zheng,Fang Junqiang,Tang Ya-jie,Wu Da-leiORCID,Wu ChangshengORCID,Li Yue-zhongORCID

Abstract

AbstractGlycosyltransferases typically display acceptor substrate flexibility but more stringent donor specificity. BsGT-1 is a highly effective glycosyltransferase to glycosylate macrolides, including epothilones, promising antitumor compounds. Here, we show that BsGT-1 has three major regions significantly influencing the glycodiversification of epothilone B based on structural molecular docking, “hot spots” alanine scanning, and site saturation mutagenesis. Mutations in the PSPG-like motif region and the C2 loop region are more likely to expand donor preference; mutations of the flexible N3 loop region located at the mouth of the substrate-binding cavity produce novel epothilone oligosaccharides. These “hot spots” also functioned in homologues of BsGT-1. The glycosides showed significantly enhanced water solubility and decreased cytotoxicity, although the glycosyl appendages of epothilone B also reduced drug permeability and attenuated antitumor efficacy. This study laid a foundation for the rational engineering of other GTs to synthesize valuable small molecules.

Funder

1.National Key Research and Development Programs of China 2.National Natural Science Foundation of China 3.the Excellent Youth Program of Shandong Natural Science Foundation

Publisher

Springer Science and Business Media LLC

Subject

General Agricultural and Biological Sciences,General Biochemistry, Genetics and Molecular Biology,Medicine (miscellaneous)

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