| Literature DB >> 29236497 |
Chafiq Hamdouchi1, Pranab Maiti2, Alan M Warshawsky1, Amy C DeBaillie1, Keith A Otto1, Kelly L Wilbur1, Steven D Kahl1, Anjana Patel Lewis1, Guemalli R Cardona1, Richard W Zink1, Keyue Chen1, Siddaramaiah Cr2, Jayana P Lineswala1, Grace L Neathery1, Cecilia Bouaichi1, Benjamin A Diseroad1, Alison N Campbell1, Stephanie A Sweetana1, Lisa A Adams1, Over Cabrera1, Xiaosu Ma1, Nathan P Yumibe1, Chahrzad Montrose-Rafizadeh1, Yanyun Chen1, Anne Reifel Miller1.
Abstract
As a part of our program to identify potent GPR40 agonists capable of being dosed orally once daily in humans, we incorporated fused heterocycles into our recently disclosed spiropiperidine and tetrahydroquinoline acid derivatives 1, 2, and 3 with the intention of lowering clearance and improving the maximum absorbable dose (Dabs). Hypothesis-driven structural modifications focused on moving away from the zwitterion-like structure. and mitigating the N-dealkylation and O-dealkylation issues led to triazolopyridine acid derivatives with unique pharmacology and superior pharmacokinetic properties. Compound 4 (LY3104607) demonstrated functional potency and glucose-dependent insulin secretion (GDIS) in primary islets from rats. Potent, efficacious, and durable dose-dependent reductions in glucose levels were seen during glucose tolerance test (GTT) studies. Low clearance, volume of distribution, and high oral bioavailability were observed in all species. The combination of enhanced pharmacology and pharmacokinetic properties supported further development of this compound as a potential glucose-lowering drug candidate.Entities:
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Year: 2018 PMID: 29236497 DOI: 10.1021/acs.jmedchem.7b01411
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446