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Non-canonical signalling and roles of the vasoactive peptides angiotensins and kinins

机译:血管活性肽血管紧张素和激肽的非典型信号传导及其作用

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GPCRs (G-protein-coupled receptors) are among the most important targets for drug discovery due to their ubiquitous expression and participation in cellular events under both healthy and disease conditions. These receptors can be activated by a plethora of ligands, such as ions, odorants, small ligands and peptides, including angiotensins and kinins, which are vasoactive peptides that are classically involved in the pathophysiology of cardiovascular events. These peptides and their corresponding GPCRs have been reported to play roles in other systems and under pathophysiological conditions, such as cancer, central nervous system disorders, metabolic dysfunction and bone resorption. More recently, new mechanisms have been described for the functional regulation of GPCRs, including the transactivation of other signal transduction receptors and the activation of G-protein-independent pathways. The existence of such alternative mechanisms for signal transduction and the discovery of agonists that can preferentially trigger one signalling pathway over other pathways (called biased agonists) have opened new perspectives for the discovery and development of drugs with a higher specificity of action and, therefore, fewer side effects. The present review summarizes the current knowledge on the non-canonical signalling and roles of angiotensins and kinins.
机译:GPCR(G蛋白偶联受体)由于其在健康和疾病条件下的普遍表达和参与细胞事件而成为药物发现的最重要目标。这些受体可以被大量的配体激活,例如离子,加味剂,小的配体和包括血管紧张素和激肽在内的肽,它们是血管活性肽,通常参与心血管事件的病理生理。据报道,这些肽及其相应的GPCR在其他系统中以及在病理生理条件下发挥作用,例如癌症,中枢神经系统疾病,代谢功能障碍和骨吸收。最近,已描述了用于GPCR功能调节的新机制,包括其他信号转导受体的反式激活和G蛋白非依赖性途径的激活。此类信号转导机制的存在以及与其他途径相比可以优先触发一种信号途径的激动剂的发现(称为“偏向激动剂”)为发现和开发具有更高作用特异性的药物开辟了新的前景,因此,副作用少。本综述总结了有关非典型信号以及血管紧张素和激肽作用的当前知识。

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