Capturing Sialyl‐glycan on Live Cancer Cells by Tailored Boronopeptide**

Author:

Chatterjee Saurav1,Chowdhury Arnab1,Saproo Sheetanshu2,Mani Tripathi Nitesh1,Naidu Srivatsava2,Bandyopadhyay Anupam1ORCID

Affiliation:

1. Biomimetic Peptide Engineering Laboratory Department of Chemistry Indian Institute of Technology Ropar 140001 Rupnagar Punjab India

2. Department of Biomedical Engineering Department of Chemistry Indian Institute of Technology Ropar 140001 Rupnagar Punjab India

Abstract

AbstractBoronic acid‐containing molecules are substantially popularized in chemical biology and medicinal chemistry due to the broad spectrum of covalent conjugations as well as interaction modules offered by the versatile boron atom. Apparently, the WGA peptide (wheat germ agglutinin, 62–73), which shows a considerably low binding affinity to sialic acid, turned into a selective and >5 folds potent binder with the aid of a suitable boronic acid probe installed chemoselectively. In silico studies prompted us to install BA probes on the cysteine residue, supposedly located in close proximity to the bound sialic acid. In vitro studies revealed that the tailored boronopeptides show enhanced binding ability due to the synergistic recognition governed by selective non‐covalent interactions and cis‐diol boronic acid conjugation. The intense binding is observed even in 10 % serum, thus enabling profiling of sialyl‐glycan on cancer cells, as compared with the widely used lectin, Sambucus nigra. The synergistic binding mode between the best boronopeptide (P3) binder and sialic acid was analyzed via 1H and 11B NMR.

Publisher

Wiley

Subject

General Chemistry,Catalysis,Organic Chemistry

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