正构和变构诱导的配体介导的gpcr转运。

Gregory J Digby, P Jeffrey Conn, Craig W Lindsley
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引用次数: 0

摘要

许多正构激动剂不同地激活gpcr的下游效应物。这种明确的信号诱导强有力地支持了被称为“配体导向的受体信号运输”(LDTRS)的假设。最近,亚型选择性GPCR激活剂,如变构激动剂和阳性变构调节剂,也显示出激活特定信号通路的能力。基于这一发现,有可能实现配体特异性受体活性状态,从而优化gpcr特异性的生物反应。这篇综述讨论了最近的研究,其中正构和变构化合物已被证明可以诱导LDTRS。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Orthosteric- and allosteric-induced ligand-directed trafficking at GPCRs.

Many orthosteric agonists differentially activate downstream effectors of GPCRs. Such defined induction of signaling has strongly supported the hypothesis termed 'ligand-directed trafficking of receptor signaling' (LDTRS). More recently, subtype-selective GPCR activators, such as allosteric agonists and positive allosteric modulators, have also exhibited the capacity to activate specific signaling pathways. Based on this finding, it may be possible to achieve ligand-specific receptor active states that optimize the biological responses specific to GPCRs. This review discusses recent studies in which both orthosteric and allosteric compounds have been demonstrated to induce LDTRS.

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