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内皮细胞上共存的两种ATP受体(P2y嘌呤受体和核苷酸受体)的异源和同源脱敏差异

Differential heterologous and homologous desensitization of two receptors for ATP (P2y purinoceptors and nucleotide receptors) coexisting on endothelial cells.

作者信息

Wilkinson G F, Purkiss J R, Boarder M R

机构信息

Department of Cell Physiology and Pharmacology, University of Leicester, UK.

出版信息

Mol Pharmacol. 1994 Apr;45(4):731-6.

PMID:8183253
Abstract

Bovine aortic endothelial cells in culture contain two coexisting phosphoinositidase C-linked receptors for ATP, the P2y-purinoceptors [for which 2-methylthio-ATP (2MeSATP) is a selective agonist] and the nucleotide (or P2u) receptors (for which UTP is a selective agonist). Here we have investigated the occurrence of homologous and heterologous desensitization of these two receptors and the involvement of protein kinase C-dependent mechanisms. Measuring total [3H]inositol (poly)phosphate accumulation in the presence of lithium, we showed that with long (15-min) stimulations with UTP or 2MeSATP desensitization occurred to a maximum of 40% within several minutes of preexposure to either agonist, i.e., with this procedure there is no difference between the heterologous and the homologous experimental design. In the remainder of the experiments reported we measured inositol-1,4,5-trisphosphate mass levels, using a protocol of 5-min preincubation, 2-min wash, and 5-sec stimulation. We found that preincubation with either agonist led to desensitization of the response to the same agonist of about 40%. However, whereas preincubation with 2MeSATP did not affect the subsequent response to UTP, preincubation with UTP did attenuate the 2MeSATP response. These results demonstrate that homologous desensitization occurs with both P2Y and nucleotide receptors but that heterologous desensitization follows only from activation of the nucleotide receptors. Preincubation with the protein kinase C inhibitor Ro 31-8220 enhanced the subsequent inositol-1,4,5-trisphosphate response to 2MeSATP but did not affect the desensitization of this response by preincubation with the same agonist. However, whereas the response to UTP was not enhanced by preincubation with the protein kinase C inhibitor, the desensitization caused by preincubation with UTP was partially inhibited by Ro 31-8220. These results show that multiple desensitizing events occur during the first few minutes of receptor activation and that these events are different for each of the receptors for ATP.

摘要

培养的牛主动脉内皮细胞含有两种与磷酸肌醇酶C相连的ATP受体,即P2y嘌呤受体[2-甲硫基ATP(2MeSATP)是其选择性激动剂]和核苷酸(或P2u)受体[UTP是其选择性激动剂]。在此,我们研究了这两种受体的同源脱敏和异源脱敏的发生情况以及蛋白激酶C依赖性机制的参与情况。在锂存在的情况下测量总的[3H]肌醇(多)磷酸积累,我们发现用UTP或2MeSATP进行长时间(15分钟)刺激时,在预先暴露于任何一种激动剂的几分钟内脱敏作用最大可达40%,也就是说,用这种方法异源和同源实验设计之间没有差异。在报告的其余实验中,我们采用5分钟预孵育、2分钟洗涤和5秒刺激的方案测量肌醇-1,4,5-三磷酸质量水平。我们发现用任何一种激动剂预孵育都会导致对相同激动剂的反应脱敏约40%。然而,虽然用2MeSATP预孵育不影响随后对UTP的反应,但用UTP预孵育确实会减弱对2MeSATP的反应。这些结果表明,P2Y和核苷酸受体都会发生同源脱敏,但异源脱敏仅由核苷酸受体的激活引起。用蛋白激酶C抑制剂Ro 31-8220预孵育可增强随后对2MeSATP的肌醇-1,4,5-三磷酸反应,但不影响用相同激动剂预孵育对该反应的脱敏作用。然而,虽然用蛋白激酶C抑制剂预孵育不会增强对UTP的反应,但Ro 31-8220可部分抑制用UTP预孵育引起的脱敏作用。这些结果表明,在受体激活的最初几分钟内会发生多种脱敏事件,并且这些事件对于每种ATP受体都是不同的。

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