MMP-13 selective α-sulfone hydroxamates: a survey of P1' heterocyclic amide isosteres.

Thomas E. Barta,Daniel P. Becker,Louis J. Bedell,Alan M. Easton,Susan L. Hockerman,James R. Kiefer,Grace E. Munie,Karl J. Mathis,Madeleine H. Li,Joseph G. Rico,Clara I. Villamil,Jennifer M. Williams

MMP-13 selective α-sulfone hydroxamates: a survey of P1' heterocyclic amide isosteres.

2011

Thomas E. Barta
Daniel P. Becker
Louis J. Bedell
Alan M. Easton
Susan L. Hockerman
James R. Kiefer
Grace E. Munie
Karl J. Mathis
Madeleine H. Li
Joseph G. Rico
Clara I. Villamil
Jennifer M. Williams

Abstract Seeking compounds preferentially potent and selective for MMP-13, we reported in the preceding Letter on a series of hydroxamic acids with a flexible benzamide tail groups. 1a Here, we replace the amide moiety with non-hydrolyzable heterocycles in an effort to improve half-life. We identify a hydroxamate tetrazole 4e that spares MMP-1 and -14, shows >400-fold selectivity versus MMP-8 and >600-fold selectivity versus MMP-2, and has a 4.8 h half-life in rats. X-ray data (1.9 A) for tetrazole 4c is presented.

Keywords:

Organic chemistry
Chemical synthesis
Selectivity
Moiety
Benzamide
Biochemistry
Amide
Hydroxamic acid
Sulfone
Tetrazole
Stereochemistry
Chemistry

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