Issue 1, 2015

Evaluation of a focused virtual library of heterobifunctional ligands for Clostridium difficile toxins

Abstract

A focused library of virtual heterobifunctional ligands was generated in silico and a set of ligands with recombined fragments was synthesized and evaluated for binding to Clostridium difficile toxins. The position of the trisaccharide fragment was used as a reference for filtering docked poses during virtual screening to match the trisaccharide ligand in a crystal structure. The peptoid, a diversity fragment probing the protein surface area adjacent to a known binding site, was generated by a multi-component Ugi reaction. Our approach combines modular fragment-based design with in silico screening of synthetically feasible compounds and lays the groundwork for future efforts in development of composite bifunctional ligands for large clostridial toxins.

Graphical abstract: Evaluation of a focused virtual library of heterobifunctional ligands for Clostridium difficile toxins

Supplementary files

Article information

Article type
Paper
Submitted
28 Aug 2014
Accepted
17 Oct 2014
First published
21 Oct 2014

Org. Biomol. Chem., 2015,13, 283-298

Author version available

Evaluation of a focused virtual library of heterobifunctional ligands for Clostridium difficile toxins

C. A. Sanhueza, J. Cartmell, A. El-Hawiet, A. Szpacenko, E. N. Kitova, R. Daneshfar, J. S. Klassen, D. E. Lang, L. Eugenio, K. K.-S. Ng, P. I. Kitov and D. R. Bundle, Org. Biomol. Chem., 2015, 13, 283 DOI: 10.1039/C4OB01838A

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