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Identification of Regions Involved in the Physical Interaction between Melanocortin Receptor Accessory Protein 2 and Prokineticin Receptor 2

机译:鉴定参与黑皮质素受体辅助蛋白 2 和促动力素受体 2 之间物理相互作用的区域

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摘要

Melanocortin Receptor Accessory Protein 2 (MRAP2) modulates the trafficking and signal transduction of several G-protein-coupled receptors (GPCRs) involved in the control of energy homeostasis, such as Prokineticin receptors (PKRs). They bind the endogenous ligand prokineticin 2 (PK2), a novel adipokine that has an anorexic effect and modulates thermoregulation and energy homeostasis. In the present work, we used biochemical techniques to analyze the mechanism of interaction of MRAP2 with PKR2 and we identified the specific amino acid regions involved in the complex formation. Our results indicate that MRAP2 likely binds to the N-terminal region of PKR2, preventing glycosylation and consequently the correct receptor localization. We also identified a C-terminal region of MRAP2 that is critical for the interaction with PKR2. Consequently, we analyzed the role of the prokineticin transduction system in the regulation of MRAP2 expression in tissues involved in the control of food intake: at the central level, in hypothalamic explants, and at the peripheral level, in adipocytes. We demonstrated the modulation of MRAP2 expression by the prokineticin transduction system.
机译:黑皮质素受体辅助蛋白 2 (MRAP2) 调节参与控制能量稳态的几种 G 蛋白偶联受体 (GPCR) 的运输和信号转导,例如促动力素受体 (PKR)。它们结合内源性配体促动力素 2 (PK2),这是一种新型脂肪因子,具有厌食作用并调节体温调节和能量稳态。在本研究中,我们利用生化技术分析了MRAP2与PKR2相互作用的机制,并确定了参与复合物形成的特定氨基酸区域。我们的结果表明,MRAP2可能与PKR2的N端区域结合,阻止糖基化,从而阻止正确的受体定位。我们还鉴定了 MRAP2 的 C 端区域,该区域对与 PKR2 的相互作用至关重要。因此,我们分析了促动力素转导系统在参与控制食物摄入的组织中调节 MRAP2 表达中的作用:在中央水平、下丘脑外植体和外周水平、脂肪细胞中。我们证明了促动力素转导系统对 MRAP2 表达的调节。

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