Dissecting Key Multivalent Processes in Glycosidase Inhibition: Insights from Thermodynamic Modelling and Atomistic Simulations

Author:

Spichty MartinORCID,Liang Yan,Schettini Rosaria,Izzo Irene,Bodlenner Anne,Compain Philippe

Abstract

AbstractMultivalency represents a powerful approach to increase the inhibition potency of moderate glycosidase inhibitors. Regarding the key role of catalytic glycoside hydrolysis in biology, understanding the molecular mechanisms and origin of the multivalent inhibitory effect is of great interest and presents a fascinating playground for theoretical studies. Our teams have recently dissected key processes of multivalent glycosidase inhibition through the use of different neoglycoclusters based on deoxynojirimycin (DNJ) inhitopes and a cyclopeptoid scaffold. This companion article details the theoretical aspects of this former study. A thermodynamic model is developed and validated, compared to literature, and extended to account for particularities of the charged DNJ inhitopes.

Publisher

Cold Spring Harbor Laboratory

Reference26 articles.

1. Glycosidase inhibitors: update and perspectives on practical use

2. Selective glycosidase inhibitors: A patent review (2012–present)

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4. Multivalency as a Chemical Organization and Action Principle

5. Note 1: The reader is referred to the companion study (ref. 5) for more details on the exact chemical structure of the clusters, their synthesis and measurements of the inhibition constants against JBα-man.

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