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Melanocortin 4 receptors interact with antimicrobial frog peptide analogues
Authors:Do Ernest U  Jo Eun Bae  Choi Gyu  Piao Long Zhu  Shin Jaekyoon  Seo Min-Duk  Kang Su-Jin  Lee Bong-Jin  Kim Kang Ho  Kim Jae Bum  Kim Su-il
Institution:School of Agricultural Biotechnology, Seoul National University, San 56-1 Sillim-dong, Gwanak-gu, Seoul 151-742, Republic of Korea.
Abstract:We have developed fluorescence polarization (FP) assays of human melanocortin 4 receptor (MC4R) in 384-well microtiter plates using TAMRA-NDP-MSH as a tracer. The rank order of potency of agonists and antagonists agrees well relative to the published assays: SHU9119>MTII>NDP alphaMSH>alphaMSH. We have screened libraries of Korean plant extracts and frog peptide analogues in search of MC4R ligands using FP assays and cell-based CRE luciferase reporter assays. We report that FLGFLFKVASK, FLGWLFKVASK, FLGALFKWASK, and FLGWLFKWASK are the peptide analogues, which bind to human MC4R receptor with good affinity in vitro. FLGWLFKVASK and FLGWLFKWASK stimulated CRE-driven reporter gene via MC4R. In luciferase reporter assays, they possess the pharmacological and functional profiles of full agonists. We demonstrate the interaction of MC4R with 11-residue antimicrobial peptides derived from the Korean frog, Rana rugosa. The results suggest that MC4R interacts promiscuously with bioactive analogues of antimicrobial peptide, gaegurin-5.
Keywords:Fluorescence polarization  High-throughput screening  Human melanocortin 4 receptors  Agonists and antagonists  Rank order of potency  Gaegurin
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