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将TRPM8鉴定为一种药效团受体。

Characterisation of TRPM8 as a pharmacophore receptor.

作者信息

Bödding Matthias, Wissenbach Ulrich, Flockerzi Veit

机构信息

Experimentelle und Klinische Pharmakologie und Toxikologie, Universität des Saarlandes, D-66421 Homburg, Germany.

出版信息

Cell Calcium. 2007 Dec;42(6):618-28. doi: 10.1016/j.ceca.2007.03.005. Epub 2007 May 22.

DOI:10.1016/j.ceca.2007.03.005
PMID:17517434
Abstract

Some proteins of the transient receptor potential (TRP) family form temperature sensitive ion channels. One member of the melastatin (M) group, namely TRPM8 is activated by cold and cooling compounds such as menthol and icilin, and its gene is up-regulated in prostate cancer and other malignancies. Here we characterise the effects of the carboxamides WS-12, CPS-113, CPS-369, the carboxylic acid WS-30 and the phosphine oxide WS-148 by Ca2+ imaging experiments and whole-cell patch-clamp recordings on TRPM8 expressing human embryonic kidney (HEK), lymph node prostate cancer (LNCaP) and dorsal root ganglia (DRG) cells. The cooling compounds introduced in this study, show a dose-dependent and reversible activation of TRPM8 with EC50 values in the nM to low microM range. The carboxamide WS-12 is most potent in activating TRPM8. It is selective, since other TRP proteins are not stimulated at muM concentrations and its efficacy with respect to TRPM8 is similar to the one of icilin. In summary, the compounds described in this study represent new tools to dissect TRPM8 functions and may serve as chemical leads for the development of additional TRPM8 agonists and novel antagonists. Such compounds may be beneficial for preventing noxious cold perception. They could also be useful in diagnosis and treatment of most common cancers in which the TRPM8 gene is up-regulated in comparison to the corresponding normal tissue.

摘要

瞬时受体电位(TRP)家族的一些蛋白质形成温度敏感离子通道。褪黑素(M)组的一个成员,即TRPM8,可被寒冷以及薄荷醇和异冰片基脲等冷却化合物激活,其基因在前列腺癌和其他恶性肿瘤中上调。在此,我们通过Ca2+成像实验以及对表达TRPM8的人胚肾(HEK)、淋巴结前列腺癌(LNCaP)和背根神经节(DRG)细胞进行全细胞膜片钳记录,来表征羧酰胺WS - 12、CPS - 113、CPS - 369、羧酸WS - 30和氧化膦WS - 148的作用。本研究中引入的冷却化合物对TRPM8表现出剂量依赖性和可逆性激活,其半数有效浓度(EC50)值在纳摩尔至低微摩尔范围内。羧酰胺WS - 12在激活TRPM8方面最为有效。它具有选择性,因为在微摩尔浓度下其他TRP蛋白未受刺激,并且其对TRPM8的功效与异冰片基脲相似。总之,本研究中描述的化合物是剖析TRPM8功能的新工具,可作为开发其他TRPM8激动剂和新型拮抗剂的化学先导物。这类化合物可能有助于预防有害的冷觉感受。它们还可能对诊断和治疗与相应正常组织相比TRPM8基因上调的最常见癌症有用。

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