Catalysts (May 2023)

Rational Design of Cyclodextrin Glycosyltransferase with Improved Hesperidin Glycosylation Activity

  • Hanchi Chen,
  • Jiajun Wang,
  • Yi Liu,
  • Yongfan Chen,
  • Chunfeng Wang,
  • Linjiang Zhu,
  • Yuele Lu,
  • Xiaolong Chen

DOI
https://doi.org/10.3390/catal13050885
Journal volume & issue
Vol. 13, no. 5
p. 885

Abstract

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Cyclodextrin glycosyltransferase (CGTase) can catalyze the glycosylation of hesperidin, resulting in α-glycosyl hesperidin with significantly improved water solubility. In this study, a rational design of CGTase to improve its hesperidin glycosylation activity was investigated. The strategy we employed involved docking hesperidin in its near-attack conformation and virtually mutating the surrounding residues, followed by calculating the changes in binding energy using Rosetta flex-ddG. The mutations with a stabilization effect were then subjected to an activity assay. Starting from CGTase-Y217F, we obtained three double-point mutants, Y217F/M351F, Y217F/M351L, and Y217F/D393H, with improved hesperidin glycosylation activities after screening twenty variants. The best variant, Y217F/D393H, exhibited a catalytic activity of 1305 U/g, and its kcat/KmA is 2.36 times higher compared to CGTase-Y217F and 15.14 times higher compared to the wild-type CGTase. Molecular dynamic simulations indicated that hesperidin was repulsed by CGTase-Y217F when bound in a near-attack conformation. However, by introducing a second-point mutation with a stabilization effect, the repulsion effect is weakened, resulting in a reduction in the distances between the bond-forming atoms and, thus, favoring the reaction.

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