Nature Communications (Oct 2024)

An efficient C-glycoside production platform enabled by rationally tuning the chemoselectivity of glycosyltransferases

  • Min Li,
  • Yang Zhou,
  • Zexing Wen,
  • Qian Ni,
  • Ziqin Zhou,
  • Yiling Liu,
  • Qiang Zhou,
  • Zongchao Jia,
  • Bin Guo,
  • Yuanhong Ma,
  • Bo Chen,
  • Zhi-Min Zhang,
  • Jian-bo Wang

DOI
https://doi.org/10.1038/s41467-024-53209-1
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 13

Abstract

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Abstract Despite the broad potential applications of C-glycosides, facile synthetic methods remain scarce. Transforming glycosyltransferases with promiscuous or natural O-specific chemoselectivity to C-glycosyltransferases is challenging. Here, we employ rational directed evolution of the glycosyltransferase MiCGT to generate MiCGT-QDP and MiCGT-ATD mutants which either enhance C-glycosylation or switch to O-glycosylation, respectively. Structural analysis and computational simulations reveal that substrate binding mode govern C-/O-glycosylation selectivity. Notably, directed evolution and mechanism analysis pinpoint the crucial residues dictating the binding mode, enabling the rational design of four enzymes with superior non-inherent chemoselectivity, despite limited sequence homology. Moreover, our best mutants undergo testing with 34 substrates, demonstrating superb chemoselectivities, regioselectivities, and activities. Remarkably, three C-glycosides and an O-glycoside are produced on a gram scale, demonstrating practical utility. This work establishes a highly selective platform for diverse glycosides, and offers a practical strategy for creating various types of glycosylation platforms to access pharmaceutically and medicinally interesting products.