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首页> 外文期刊>Current Neuropharmacology >Human 5-HT4 and 5-HT7 Receptor Splice Variants: Are they Important?
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Human 5-HT4 and 5-HT7 Receptor Splice Variants: Are they Important?

机译:人类5-HT4和5-HT7受体剪接变体:它们重要吗?

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摘要

-protein-coupled receptors (GPCRs), which are encoded by > 300 genes in the human genome, are by far the largest class of targets for modern drugs. These macromolecules display inherent adaptability of function, which is partly due to the production of different forms of the receptor protein. These are commonly called ‘isoforms’ or ‘splice variants’ denoting the molecular process of their production/ assembly. Not all GPCRs are expressed as splice variants, but certain subclasses of 5-HT receptors are for example, the 5-HT4 and 5-HT7 receptors. There are at least 11 human 5-HT4 and three h5-HT7 receptor splice variants. This review describes their discoveries, nomenclature and structures. The discovery that particular splice variants are tissue specific (or prominent) has highlighted their potential as future drug targets. In particular, this review examines the functional relevance of different 5-HT4 and 5-HT7 receptor splice variants. Examples are given to illustrate that splice variants have differential modulatory influences on signalling processes. Differences in agonist potency and efficacies and also differences in desensitisation rates to 5-HT occur with both 5-HT4 and 5-HT7 receptor splice variants. The known and candidate signalling systems that allow for splice variant specific responses include GPCR interacting proteins (GIPs) and GPCR receptor kinases (GRKs) which are examined. Finally, the relevance of 5-HT receptor splice variants to clinical medicine and to the pharmaceutical industry is discussed.
机译:-蛋白偶联受体(GPCR)由人类基因组中的300多个基因编码,是现代药物的最大靶标。这些大分子显示出固有的功能适应性,部分原因是产生不同形式的受体蛋白。这些通常称为“异构体”或“剪接变体”,表示其生产/组装的分子过程。并非所有的GPCR都表达为剪接变体,但是5-HT受体的某些亚类是例如5-HT4和5-HT7受体。至少有11个人类5-HT4和三个h5-HT7受体剪接变体。这篇评论描述了他们的发现,术语和结构。特定剪接变体具有组织特异性(或突出性)的发现突出了其作为未来药物靶标的潜力。特别地,该综述检查了不同的5-HT 4和5-HT 7受体剪接变体的功能相关性。给出实例来说明剪接变体对信号传导过程具有不同的调制影响。对于5-HT 4和5-HT 7受体剪接变体,激动剂效力和功效的差异以及对5-HT的脱敏速率的差异也发生。允许剪接变体特异性反应的已知和候选信号系统包括已检查的GPCR相互作用蛋白(GIP)和GPCR受体激酶(GRK)。最后,讨论了5-HT受体剪接变体与临床医学和制药工业的相关性。

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