首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Cell Surface Targeting Of μ-δ Opioid Receptor Heterodimers By Rtp4
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Cell Surface Targeting Of μ-δ Opioid Receptor Heterodimers By Rtp4

机译:Rtp4对μ-δ阿片受体异二聚体的细胞表面靶向

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摘要

μ opioid receptors are G protein-coupled receptors that mediate the pain-relieving effects of clinically used analgesics, such as morphine. Accumulating evidence shows that μ-δ opioid heterodimers have a pharmacologic profile distinct from those of the μ or δ homodimers. Because the heterodimers exhibit distinct signaling properties, the protein and mechanism regulating their levels have significant effects on morphine-mediated physiology. We report the characterization of RTP4, a Golgi chaperone, as a regulator of the levels of heterodimers at the cell surface. We show that the association with RTP4 protectsμ-δ receptors from ubiq-uitination and degradation. This leads to increases in surface heterodimer levels, thereby affecting signaling. Thus, the oligo-meric organization of opioid receptors is controlled by RTP4, and this governs their membrane targeting and functional activity. This work is the first report of the identification of a chaperone involved in the regulation of the biogenesis of a family A GPCR heterodimer. The identification of such factors as RTP4 controlling dimerization will provide insight into the regulation of heterodimers in vivo. This has implications in the modulation of pharmacology of their endogenous ligands, and in the development of drugs with specific therapeutic effects.
机译:μ阿片样物质受体是G蛋白偶联受体,可介导临床使用的止痛药(例如吗啡)的止痛作用。越来越多的证据表明,μ-δ阿片类异二聚体的药理特性与μ或δ同二聚体的药理特性不同。由于异二聚​​体表现出独特的信号传导特性,因此蛋白质及其调节其水平的机制对吗啡介导的生理学具有重要影响。我们报告RTP4,高尔基分子伴侣,作为在细胞表面的异二聚体水平的调节剂的表征。我们表明与RTP4的关联保护μδ受体免受泛素化和降解。这导致表面异二聚体水平增加,从而影响信号传导。因此,阿片受体的低聚组织受RTP4的控制,这控制着它们的膜靶向和功能活性。这项工作是鉴定伴侣蛋白A家庭GPCR异源二聚体调控的第一份报告。诸如RTP4控制二聚化等因素的鉴定将提供对体内异二聚体调节的见解。这对调节其内源性配体的药理作用和开发具有特定治疗作用的药物有影响。

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