Old molecules for new receptors:: Trp(Nps) dipeptide derivatives as vanilloid TRPV1 channel blockers

被引:10
|
作者
Angeles Bonache, M.
Garcia-Martinez, Carolina
Garcia de Diego, Laura
Carreno, Cristina
Perez de Vega, M. Jesus
Garcia-Lopez, M. Teresa
Ferrer-Montiel, Antonio
Gonzalez-Muniz, Rosario
机构
[1] Instituto de Química Médica (CSIC), Juan de la Cierva, Madrid
关键词
D O I
10.1002/cmdc.200500094
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
The transient receptor potential vanilloid member I (TRPV1), an integrator of multiple pain-producing stimuli, is regarded nowadays as an important biological target for the discovery of novel analgesics. Here, we describe the first experimental evidence for the behavior of an old family of analgesic dipeptides, namely Xaa-Trp(Nps) and Trp(Nps)-Xaa (Xaa=Lys, Arg) derivatives, as potent TRPV1 channel blockers. We also report the synthesis and biological investigation of a series of new conformationally restricted Trp(Nps)-dipeptide derivatives with improved TRPV1/ NMDA selectivity. Compound 15b, which incorporates an N-terminal 2S-azetidine-derived Arg residue, was the most selective compound in this series. Collectively, a new family of TRPV1 channel blockers emerged from our results, although further modifications are required to fine-tune the potency/selectivity/ toxicity balance.
引用
收藏
页码:429 / 438
页数:10
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