Native MS: an ’ESI‚ way to support structure- and fragment-based drug discovery

Author:

Vivat Hannah Valerie1,Atmanene C2,Zeyer D1,Van Dorsselaer A2,Sanglier-Cianférani Sarah2

Affiliation:

1. NovAliX Structural Biology, Bioparc, Boulevard Sebastien Brant, Illkirch 67400, France.

2. Laboratoire de Spectrométrie de Masse BioOrganique, IPHC-DSA, CNRS UMR7178, Université de Strasbourg UdS, Strasbourg 67087, France.

Abstract

The success of early drug-discovery programs depends on the adequate combination of complementary and orthogonal technologies allowing hit/lead compounds to be optimized and improve therapeutic activity. Among the available biophysical methods, native MS recently emerged as an efficient method for compound-binding screening. Native MS is a highly sensitive and accurate screening technique. This review provides a description of the general approach and an overview of the possible characterization of ligand-binding properties. How native MS supports structure- and fragment-based drug research will also be discussed, with examples from the literature and internal developments. Native MS shows strong potential for in-depth characterization of ligand-binding properties. It is also a reliable screening technique in drug-discovery processes.

Publisher

Future Science Ltd

Subject

Drug Discovery,Pharmacology,Molecular Medicine

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