Discovery of a small molecule RXFP3/4 agonist that increases food intake in rats upon acute central administration |
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| Authors: | Brian DeChristopher Soo-Hee Park Linh Vong Derek Bamford Hyun-Hee Cho Rohit Duvadie Allison Fedolak Christopher Hogan Toshiyuki Honda Pramod Pandey Olga Rozhitskaya Liansheng Su Elizabeth Tomlinson Iain Wallace |
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| Institution: | Novartis Institutes for BioMedical Research, 250 Massachusetts Avenue, Cambridge, MA 02139, United States |
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| Abstract: | The relaxin family peptide receptors have been implicated in numerous physiological processes including energy homeostasis, cardiac function, wound healing, and reproductive function. Two family members, RXFP3 and RXFP4, are class A GPCRs with endogenous peptide ligands (relaxin-3 and insulin-like peptide 5 (INSL5), respectively). Polymorphisms in relaxin-3 and RXFP3 have been associated with obesity, diabetes, and hypercholesterolemia. Moreover, central administration of relaxin-3 in rats has been shown to increase food intake, leading to body weight gain. Reported RXFP3 and RXFP4 ligands have been restricted to peptides (both endogenous and synthetic) as well as a low molecular weight positive allosteric modulator requiring a non-endogenous orthosteric ligand. Described here is the discovery of the first potent low molecular weight dual agonists of RXFP3/4. The scaffold identified is competitive with a chimeric relaxin-3/INSL5 peptide for RXFP3 binding, elicits similar downstream signaling as relaxin-3, and increases food intake in rats following acute central administration. This is the first report of small molecule RXFP3/4 agonism. |
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| Keywords: | RXFP3 RXFP4 Relaxin-3 Insulin-like peptide |
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