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Discovery of a Novel, Selective, and Orally Bioavailable Class of Thrombin Inhibitors Incorporating Aminopyridyl Moieties at the P1 Position

Authors :
Shi-Shan Mao
E P Baskin
Julie A. Krueger
Mark G. Bock
Dong-Mei Feng
A. M. Mulichak
Stephen J. Gardell
Roger M. Freidinger
Lucas R
Ramjit Hg
Jules A. Shafer
S. D. Lewis
R Woltmann
K B Dancheck
Timothy R. Hare
J.J. Lynch
Adel M. Naylor-Olsen
I.-W. Chen
Zhongguo Chen
Joe P. Vacca
Source :
Journal of Medicinal Chemistry. 40:3726-3733
Publication Year :
1997
Publisher :
American Chemical Society (ACS), 1997.

Abstract

A novel class of thrombin inhibitors incorporating aminopyridyl moieties at the P1 position has been discovered. Four of these thrombin inhibitors (13b,c,e and 14d) showed nanomolar potency (Ki 0.8-12 nM), 300-1500-fold selectivity for thrombin compared with trypsin, and good oral bioavailability (F = 40-76%) in rats or dogs. The neutral P1 was expected to increase metabolic stability and oral absorption. Identification of this novel aminopyridyl group at P1 was a key step in our search for a clinical candidate.

Subjects

Subjects :
Pyridines
Stereochemistry
Administration, Oral
Biological Availability
Peptide
Crystallography, X-Ray
Chemical synthesis
Antithrombins
Structure-Activity Relationship
Dogs
Thrombin
Drug Discovery
medicine
Animals
Structure–activity relationship
chemistry.chemical_classification
biology
Chemistry
Dipeptides
Trypsin
Rats
Kinetics
Enzyme
Enzyme inhibitor
biology.protein
Molecular Medicine
medicine.drug
Discovery and development of direct thrombin inhibitors

Details

ISSN :
15204804 and 00222623
Volume :
40
Database :
OpenAIRE
Journal :
Journal of Medicinal Chemistry
Accession number :
edsair.doi.dedup.....c1a9c3eb4d8f15436d50d759edace5a6
Full Text :
https://doi.org/10.1021/jm970493r
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