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首页> 外文期刊>Peptides: An International Journal >Discrimination of galanin receptor subtypes in RINm5F cells by structurally different galanin radioligands.
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Discrimination of galanin receptor subtypes in RINm5F cells by structurally different galanin radioligands.

机译:通过结构上不同的甘丙肽放射性配体区分RINm5F细胞中的甘丙肽受体亚型。

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摘要

Galanin (GAL) is a biologically active peptide that is involved in a variety of physiological functions. The purpose of this study was to evaluate whether porcine and rat galanin radioligands could be used as probes to discriminate GAL receptors (GALR) subtypes using a cell line, RINm5F, that express multiple GALR subtypes. Data from parallel equilibrium binding experiments using the same RINm5F membrane homogenates reveal that [125I]pGAL labels 20% more GALRs with a 2-fold lower affinity than those values identified when using [125I]rGAL. Competition studies using various GAL peptides showed different rank order of potencies depending on the radioligand used. Preincubation of RINm5F membranes with GppNHp, a non-hydrolizable GTP analog, prior to radioligand labeling suggests that a portion of GALRs is precoupled to G proteins. In addition, receptors labeled by [125I]rGAL appear more sensitive to GppNHp-induced uncoupling of G proteins than those labeled by [125I]pGAL. In conclusion, our data suggest that pGAL and rGAL radioligands define different pharmacological profiles of GALRs, and hence, these ligands can be used as pharmacological tools to discriminate GALR subtypes. Additionally, our data suggests that GALRs exist in a precoupled state with their respective G-proteins prior to interaction with the agonist.
机译:甘丙肽(GAL)是一种生物活性肽,参与多种生理功能。这项研究的目的是评估是否使用猪和大鼠甘丙肽放射配体作为探针,使用表达多种GALR亚型的细胞系RINm5F来识别GAL受体(GALR)亚型。使用相同的RINm5F膜匀浆进行的平行平衡结合实验的数据表明,与使用[125I] rGAL鉴定的那些值相比,[125I] pGAL标记的GALRs多20%,亲和力低2倍。使用各种GAL肽的竞争研究表明,根据所用放射性配体的不同,效力的等级顺序也不同。在放射性配体标记之前,将RINm5F膜与GppNHp(一种不可水解的GTP类似物)一起预孵育,表明部分GALRs已与G蛋白预偶联。此外,与[125I] pGAL标记的受体相比,[125I] rGAL标记的受体对GppNHp诱导的G蛋白解偶联更敏感。总之,我们的数据表明pGAL和rGAL放射性配体定义了GALR的不同药理学特征,因此,这些配体可用作区分GALR亚型的药理学工具。另外,我们的数据表明GALRs在与激动剂相互作用之前与它们各自的G蛋白以预偶联状态存在。

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