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首页> 外文期刊>CNS & neurological disorders drug targets >Prime time for G-protein-coupled receptor heteromers as therapeutic targets for CNS disorders: the dopamine D-D receptor heteromer.
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Prime time for G-protein-coupled receptor heteromers as therapeutic targets for CNS disorders: the dopamine D-D receptor heteromer.

机译:G蛋白偶联受体异聚体作为中枢神经系统疾病治疗靶点的黄金时间:多巴胺D-D受体异聚体。

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摘要

A number of G-protein-coupled receptors (GPCRs) are currently under consideration as potential therapeutic targets for drugs acting in the central nervous system (CNS). Attempts to discover new medications have operated under the assumption that GPCRs are monomers and that a specific drug activates one single receptor coupled to one single signal transduction mechanism. In the neuronal membrane, GPCRs are now known to be arranged into homo- and hetero-oligomers; drugs acting on a single receptor within a specific heteromer context are thought to induce a particular downstream signaling. However, there is recent evidence showing that heteromer-tailored drugs can be designed that display different affinities for a given receptor depending on the receptor partners contained within the heteromer. It can therefore be predicted that customized drugs targeting a specific receptor heteromer in the CNS might improve safety and efficacy for their therapeutic targets. Finally, it will be important to identify receptor heteromers that are involved in the pathogenesis of diseases, such as the recently discovered dopamine D-D receptor heteromer, which might play a key role in L-DOPA-induced dyskinesia in Parkinson's disease.
机译:当前,许多G蛋白偶联受体(GPCR)正在考虑作为作用于中枢神经系统(CNS)的药物的潜在治疗靶标。尝试发现新药物的假设是,GPCR是单体,一种特定药物会激活与一个信号转导机制偶联的一个受体。现在已知在神经元膜中,GPCR被排列成同聚和异聚寡聚体。在特定异聚体环境下作用于单个受体的药物被认为诱导特定的下游信号传导。然而,最近的证据表明,可以设计针对异源受体的异源药物,取决于异源分子中所含的受体伴侣,它对给定的受体表现出不同的亲和力。因此可以预见,靶向CNS中特定受体异源单体的定制药物可能会提高其治疗靶标的安全性和功效。最后,鉴定参与疾病发病机制的受体异聚体非常重要,例如最近发现的多巴胺D-D受体异聚体,其可能在帕金森氏病的L-DOPA诱导的运动障碍中起关键作用。

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