Discovery of highly potent Src SH2 binders: structure-activity studies and X-ray structures

Pierre Deprez; Isabelle Baholet; Stéphane Burlet; Gudrun Lange; Remi Amengual; Bernard Schoot; Annie Vermond; Eliane Mandine; Dominique Lesuisse

doi:10.1016/s0960-894x(02)00139-7

Discovery of highly potent Src SH2 binders: structure-activity studies and X-ray structures

Bioorg Med Chem Lett. 2002 May 6;12(9):1291-4. doi: 10.1016/s0960-894x(02)00139-7.

Authors

Pierre Deprez¹, Isabelle Baholet, Stéphane Burlet, Gudrun Lange, Remi Amengual, Bernard Schoot, Annie Vermond, Eliane Mandine, Dominique Lesuisse

Affiliation

¹ Aventis Pharma, Paris Research Center, Medicinal Chemistry, 102 route de Noisy, 93235 Cedex, Romainville, France. pierre.deprez@aventis.com

PMID: 11965373
DOI: 10.1016/s0960-894x(02)00139-7

Abstract

Optimization of the hydrophobic moiety of caprolactam/thiazepinone based compounds led to the identification of potent Src SH2 binders in two different series incorporating a phosphotyrosine group (RU 81843) or a phosphobenzoic group (RU 79181). The X-ray co-structures with the Src SH2 domain revealed different binding modes for RU 81843 and RU 79181, and an excellent fit between RU81843 and the Src SH2 protein thus explaining its high potency (9 nM, 15-fold more potent than pYEEI reference peptide).

MeSH terms

Benzoates / chemistry
Benzoates / metabolism*
Caprolactam / analogs & derivatives
Caprolactam / chemistry
Caprolactam / metabolism*
Molecular Structure
Organophosphorus Compounds / chemistry
Organophosphorus Compounds / metabolism*
Phosphotyrosine / analogs & derivatives
Phosphotyrosine / chemistry
Phosphotyrosine / metabolism*
Structure-Activity Relationship
X-Ray Diffraction
src Homology Domains*

Substances

Benzoates
Organophosphorus Compounds
RU 79181
RU 81843
Phosphotyrosine
Caprolactam