| Literature DB >> 26683635 |
Bi-Oh Park1, Seong Heon Kim2, Gye Yeong Kong1, Da Hui Kim1, Mi So Kwon3, Su Ui Lee4, Mun-Ock Kim4, Sungchan Cho2, Sangku Lee5, Hyun-Jun Lee4, Sang-Bae Han6, Young Shin Kwak7, Sung Bae Lee8, Sunhong Kim9.
Abstract
GPR43/Free Fatty Acid Receptor 2 (FFAR2) is known to be activated by short-chain fatty acids and be coupled to Gi and Gq family of heterotrimeric G proteins. GPR43 is mainly expressed in neutrophils, adipocytes and enteroendocrine cells, implicated to be involved in inflammation, obesity and type 2 diabetes. However, several groups have reported the contradictory data about the physiological functions of GPR43, so that its roles in vivo remain unclear. Here, we demonstrate that a novel compound of pyrimidinecarboxamide class named as BTI-A-404 is a selective and potent competitive inverse agonist of human GPR43, but not the murine ortholog. Through structure-activity relationship (SAR), we also found active compound named as BTI-A-292. These regulators increased the cyclic AMP level and reduced acetate-induced cytoplasmic Ca(2+) level. Furthermore, we show that they modulated the downstream signaling pathways of GPR43, such as ERK, p38 MAPK, and NF-κB. It was surprising that two compounds augmented the secretion of glucagon-like peptide 1 (GLP-1) in NCI-H716 cell line. Collectively, these novel and specific competitive inhibitors regulate all aspects of GPR43 signaling and the results underscore the therapeutic potential of them.Entities:
Keywords: Acetate (Pubchem CID:176); BTI-A-202; BTI-A-404; CATPB (Pubchem CID:53308747); GLP-1; GPR43; Inverse agonist; Propionate (Pubchem CID:1032); SCFA
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Year: 2015 PMID: 26683635 DOI: 10.1016/j.ejphar.2015.12.010
Source DB: PubMed Journal: Eur J Pharmacol ISSN: 0014-2999 Impact factor: 4.432