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The atypical chemokine receptor ACKR3/CXCR7 is a broad-spectrum scavenger for opioid peptides

机译:非典型趋化因子受体Ackr3 / CXCR7是阿片类药物的广谱清除剂

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Endogenous opioid peptides and prescription opioid drugs modulate pain, anxiety and stress by activating opioid receptors, currently classified into four subtypes. Here we demonstrate that ACKR3/CXCR7, hitherto known as an atypical scavenger receptor for chemokines, is a broad-spectrum scavenger of opioid peptides. Phylogenetically, ACKR3 is intermediate between chemokine and opioid receptors and is present in various brain regions together with classical opioid receptors. Functionally, ACKR3 is a scavenger receptor for a wide variety of opioid peptides, especially enkephalins and dynorphins, reducing their availability for the classical opioid receptors. ACKR3 is not modulated by prescription opioids, but we show that an ACKR3-selective subnanomolar competitor peptide, LIH383, can restrain ACKR3's negative regulatory function on opioid peptides in rat brain and potentiate their activity towards classical receptors, which may open alternative therapeutic avenues for opioid-related disorders. Altogether, our results reveal that ACKR3 is an atypical opioid receptor with cross-family ligand selectivity.
机译:内源性阿片类药物和处方阿片类药物通过激活阿片受体调节疼痛,焦虑和应力,目前分为四个亚型。在这里,我们证明Ackr3 / CXCR7,其被称为趋化因子的非典型清除剂受体,是阿片类药物肽的广谱清除剂。系统发育地,AckR3是趋化因子和阿片受体之间的中间体,并与典型的阿片受体一起存在于各种脑区域中。在功能上,Ackr3是一种清除剂受体,用于各种阿片类药物肽,尤其是enkephalins和Dynorphins,降低了典型阿片受体的可用性。 Ackr3未被处方阿片类药物调节,但我们表明Ackr3选择性亚诺莫醇竞争肽LiH383可以抑制大鼠脑中的阿片类肽的Ackr3的阴性调节功能,并将其活性朝向古典受体中的活性,这可能为阿片类药物打开替代治疗途径 - 相关的障碍。完全,我们的结果表明Ackr3是一种非典型阿片受体,具有交叉家庭配体选择性。

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