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Complexing Receptor Pharmacology:Modulation of Family B G Protein—Coupled Receptor Function by RAMPs

机译:络合受体药理学:通过斜坡调节FALICE B G蛋白偶联受体功能

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The most well-characterized subgroup of family B G protein—coupledreceptors (GPCRs) comprises receptors for peptide hormones, such as secretin, calcitonin (CT), glucagon, and vasoactive intestinal peptide (VIP). Recent data suggest that many of these receptors can interact with a novel family of GPCR accessory proteins termed receptor activity modifying proteins (RAMPs). RAMP interaction with receptors can lead to a variety of actions that include chaperoning of the receptor protein to the cell surface as is the case for the calcitonin receptor-like receptor (CLR) and the generation of novel receptor phenotypes. RAMP heterodimerization with the CLR and related CT receptor is required for the formation of specific CT gene-related peptide, adrenomedullin (AM) or amylin receptors. More recent work has revealed that the specific RAMP present in a heterodimer may modulate other functions such as receptor internalization and recycling and also the strength of activation of downstream signaling pathways. In this article we review our current state of knowledge of the consequence of RAMP interaction with family B GPCRs.
机译:家庭B g蛋白偶联剂(GPCR)的最良好表征亚组包含肽激素的受体,例如棘蛋白,降钙素(CT),胰高血糖素和血管活性肠肽(VIP)。最近的数据表明,许多这些受体可以与称为受体活性改性蛋白(斜坡)称为受体活性的新型GPCR辅助蛋白质。与受体的斜坡相互作用可以导致各种动作,包括对细胞表面的受体蛋白的陪伴而言,因为转析素受体样受体(CLR)和新的受体表型的产生。需要与CLR和相关CT受体形成特异性CT基因相关肽,肾上腺素髓素(AM)或淀粉蛋白受体所需的斜坡异二聚体。最近的工作表明,存在于异二聚体中的特定斜坡可以调节其他功能,例如受体内化和再循环,以及下游信号传导途径的激活强度。在本文中,我们审查了我们目前的知识状态,了解与家庭B GPCR的斜坡互动的结果。

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