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Functional selectivity of adenosine receptor ligands

机译:腺苷受体配体的功能选择性

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Adenosine receptors are plasma membrane proteins that transduce an extracellular signal into the interior of the cell. Basically every mammalian cell expresses at least one of the four adenosine receptor subtypes. Recent insight in signal transduction cascades teaches us that the current classification of receptor ligands into agonists, antagonists, and inverse agonists relies very much on the experimental setup that was used. Upon activation of the receptors by the ubiquitous endogenous ligand adenosine they engage classical G protein-mediated pathways, resulting in production of second messengers and activation of kinases. Besides this well-described G protein-mediated signaling pathway, adenosine receptors activate scaffold proteins such as β-arrestins. Using innovative and sensitive experimental tools, it has been possible to detect ligands that preferentially stimulate the β-arrestin pathway over the G protein-mediated signal transduction route, or vice versa. This phenomenon is referred to as functional selectivity or biased signaling and implies that an antagonist for one pathway may be a full agonist for the other signaling route. Functional selectivity makes it necessary to redefine the functional properties of currently used adenosine receptor ligands and opens possibilities for new and more selective ligands. This review focuses on the current knowledge of functionally selective adenosine receptor ligands and on G protein-independent signaling of adenosine receptors through scaffold proteins.
机译:腺苷受体是质膜蛋白,可将细胞外信号转导到细胞内部。基本上,每个哺乳动物细胞都表达四种腺苷受体亚型中的至少一种。信号转导级联的最新见解告诉我们,受体配体的当前分类为激动剂,拮抗剂和反向激动剂非常依赖于所使用的实验装置。在普遍存在的内源性配体腺苷激活受体后,它们会参与经典的G蛋白介导的途径,从而产生第二信使并激活激酶。除了这个众所周知的G蛋白介导的信号传导途径外,腺苷受体还激活诸如β-arrestin之类的支架蛋白。使用创新且灵敏的实验工具,有可能检测到比G蛋白介导的信号转导途径优先刺激β-arrestin途径的配体,反之亦然。这种现象被称为功能选择性或偏向信号传导,意味着一种途径的拮抗剂可能是另一种信号途径的完全激动剂。功能选择性使得必须重新定义当前使用的腺苷受体配体的功能性质,并为新的和更具选择性的配体打开了可能性。这篇综述集中于功能选择性腺苷受体配体的当前知识和腺苷受体通过支架蛋白的G蛋白非依赖性信号传导。

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