Issue 10, 2018, Issue in Progress

Probing the stereoselectivity of OleD-catalyzed glycosylation of cardiotonic steroids

Abstract

The glycosyltransferase OleD variant as a catalyst for the glycosylation of four pairs of epimers of cardiotonic steroids (CTS) are assessed. The results of this study demonstrated that the OleD-catalyze glycosylation of CTS is significantly influenced by the configuration at C-3 and the A/B fusion mode. 3β-OH and A/B ring cis fusion are favoured by OleD (ASP). An epoxide ring at C-14 and C-15 further increases the bioconversion rate; while an acetyl group at C-16 and lactone ring type at C-17 did not influence the biotransformation. A high conversion rate corresponded to a low Km value. A molecular docking simulation showed that filling of hydrophobic pocket II and interaction with residue Tyr115 may play an important role in the glycosylation reactions catalyzed by OleD glycosyltransferases. Furthermore, the glycosylation products showed a stronger inhibitory activity for Na+, K+-ATPase than the corresponding aglycones. This study provides the first stereoselective properties for OleD (ASP) catalyzed glycosylation.

Graphical abstract: Probing the stereoselectivity of OleD-catalyzed glycosylation of cardiotonic steroids

Supplementary files

Article information

Article type
Paper
Submitted
01 Nov 2017
Accepted
16 Jan 2018
First published
30 Jan 2018
This article is Open Access
Creative Commons BY license

RSC Adv., 2018,8, 5071-5078

Probing the stereoselectivity of OleD-catalyzed glycosylation of cardiotonic steroids

X. Zhu, C. Wen, Q. Ye, W. Xu, D. Zou, G. Liang, F. Zhang, W. Chen and R. Jiang, RSC Adv., 2018, 8, 5071 DOI: 10.1039/C7RA11979H

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