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垂体腺苷酸环化酶激活肽(PACAP)受体的选择性剪接有助于 PACAP-27 的功能。

Alternative splicing of the pituitary adenylate cyclase-activating polypetide (PACAP) receptor contributes to function of PACAP-27.

机构信息

Department of Pharmacology, Graduate School of Medical and Dental Sciences, Kagoshima University, Sakuragaoka, Kagoshima, Japan.

出版信息

J Mol Neurosci. 2010 Nov;42(3):341-8. doi: 10.1007/s12031-010-9385-2. Epub 2010 May 15.

Abstract

Pituitary adenylate cyclase-activating polypeptide (PACAP)-27 and PACAP-38 are neuropeptides performing a variety of physiological functions. The PACAP-specific receptor PAC1 has several variants that result mainly from alternative splicing in the mRNA region encoding the first extracellular (EC1) domain and the third intracellular cytoplasmic (IC3) loop. To characterize the molecular forms of alternative splicing variants of PAC1, we examined the binding affinity and activation of two major second messenger pathways (cAMP production and changes in Ca(2+)) by PACAP-27. Activation of cAMP was influenced by the variant in both of the EC1 domain and IC3 loops. In the N form in the EC1 domain, the suppressive effect of the HOP1 form in the IC3 loop was enhanced. Regarding the intracellular calcium mobilization assay, the rank order of the potency of PACAP-27 for the different PAC1 isoforms was S/HOP1>>N/R~S/R>>N/HOP1. In particular, PACAP-27 exhibited remarkable potency of calcium mobilization in the S/HOP1-expressing cells at sub-picomolar concentrations even though the affinities of PACAP-27 to the four PAC1 isoforms were not significantly different. This suggests the specific functions of PACAP-27 due to PACAP-27 preferring PAC1 activation, and leads in clarification of the pleiotoropic function of PACAP.

摘要

垂体腺苷酸环化酶激活肽(PACAP)-27 和 PACAP-38 是具有多种生理功能的神经肽。PACAP 特异性受体 PAC1 有几种变体,主要是由编码第一细胞外(EC1)域和第三细胞内细胞质(IC3)环的 mRNA 区域的选择性剪接产生的。为了研究 PAC1 选择性剪接变体的分子形式,我们研究了 PACAP-27 对两种主要第二信使途径(cAMP 产生和 Ca(2+)变化)的结合亲和力和激活作用。EC1 域和 IC3 环中的变体都影响 cAMP 的激活。在 EC1 域中的 N 形式中,IC3 环中的 HOP1 形式的抑制作用增强。关于细胞内钙动员测定,不同 PAC1 同工型对 PACAP-27 的效力顺序为 S/HOP1>>N/R~S/R>>N/HOP1。特别是,PACAP-27 在 S/HOP1 表达细胞中以亚皮摩尔浓度表现出显著的钙动员能力,尽管 PACAP-27 对四种 PAC1 同工型的亲和力没有显著差异。这表明 PACAP-27 由于 PACAP-27 优先激活 PAC1 而具有特定的功能,并阐明了 PACAP 的多效性功能。

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