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嵌合型M2/M5毒蕈碱受体的组成性激活及G蛋白偶联选择性结构域的描绘

Constitutive activation of chimeric m2/m5 muscarinic receptors and delineation of G-protein coupling selectivity domains.

作者信息

Burstein E S, Spalding T A, Brann M R

机构信息

Department of Psychiatry, University of Vermont, Burlington 05405, USA.

出版信息

Biochem Pharmacol. 1996 Feb 23;51(4):539-44. doi: 10.1016/0006-2952(95)02234-1.

Abstract

To derive structure/function relationships for muscarinic receptor/G-protein coupling, the m2 and m5 muscarinic receptors and a series of m2/m5 chimeras were tested for agonist binding and functional responses in a cellular proliferation/transformation assay. m5, which mediates stimulation of phosphatidylinositol turnover, displayed robust activity in the proliferation assay, whereas m2, which mediates inhibition of adenylyl cyclase, was inactive in the proliferation assay. Chimeras that contained m2 sequences in the i2 or i3 loops had impaired activity or were inactive, respectively. Chimeras that contained m2 segments reaching from the N-terminus to TM2, or from TM6 to the C-terminus, had enhanced activity relative to m5, and a chimera with both of these elements was constitutively activated.

摘要

为了推导毒蕈碱受体与G蛋白偶联的结构/功能关系,我们在细胞增殖/转化试验中测试了m2和m5毒蕈碱受体以及一系列m2/m5嵌合体的激动剂结合和功能反应。介导磷脂酰肌醇周转率刺激的m5在增殖试验中表现出强大的活性,而介导腺苷酸环化酶抑制的m2在增殖试验中无活性。在i2或i3环中包含m2序列的嵌合体活性受损或分别无活性。包含从N端到TM2或从TM6到C端的m2片段的嵌合体相对于m5具有增强的活性,并且具有这两个元件的嵌合体被组成性激活。

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