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自发性高血压大鼠血小板中增强的磷酸肌醇代谢与细胞反应之间的关系。

Relationship between enhanced phosphoinositide turnover and cellular responses in platelets from spontaneously hypertensive rats.

作者信息

Koutouzov S, Remmal A, Meyer P, Marche P

机构信息

INSERM U7, Department of Pharmacology, Hospital Necker, Paris, France.

出版信息

J Cardiovasc Pharmacol. 1988;11 Suppl 1:S6-9.

PMID:2459517
Abstract

Thrombin-induced aggregation and serotonin release were markedly enhanced in platelets from spontaneously hypertensive rats (SHR) when compared to normotensive Wistar-Kyoto (WKY) controls. Since phosphoinositides are involved in calcium-mediated platelet responses, the metabolism of these lipids was investigated in SHR and WKY rats by using 32P-labeled quiescent platelets. In unstimulated cells, both the rate and extent of 32P incorporation into individual inositol-containing phospholipids and phosphatidic acid (PA) were identical in SHR and WKY rats. This suggests that the pool size and basal turnover of phosphoinositides did not differ between the two strains. In contrast, early thrombin-induced phosphoinositide metabolism, when monitored as changes in 32P-PA, was significantly higher in SHR than in WKY rats. Following thrombin stimulation, 32P-PA formation likely reflects the initial agonist-receptor interaction; therefore, our results suggest that phospholipase C activity is enhanced in SHR platelets. Thus, it can be postulated that the observed hypersensitivity of SHR phospholipase C may play a role in the overall alteration of cell calcium handling and hence in the SHR platelet response.

摘要

与正常血压的Wistar-Kyoto(WKY)对照大鼠相比,自发性高血压大鼠(SHR)血小板中凝血酶诱导的聚集和5-羟色胺释放明显增强。由于磷酸肌醇参与钙介导的血小板反应,因此通过使用32P标记的静息血小板,在SHR和WKY大鼠中研究了这些脂质的代谢。在未刺激的细胞中,SHR和WKY大鼠中32P掺入单个含肌醇磷脂和磷脂酸(PA)的速率和程度相同。这表明两种品系之间磷酸肌醇的库大小和基础周转率没有差异。相反,当以32P-PA的变化监测时,早期凝血酶诱导的磷酸肌醇代谢在SHR中明显高于WKY大鼠。凝血酶刺激后,32P-PA的形成可能反映了最初的激动剂-受体相互作用;因此,我们的结果表明SHR血小板中磷脂酶C活性增强。因此,可以推测观察到的SHR磷脂酶C的超敏反应可能在细胞钙处理的整体改变中起作用,从而在SHR血小板反应中起作用。

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Hypersensitivity of phospholipase C in platelets of spontaneously hypertensive rats.
Hypertension. 1987 Nov;10(5):497-504. doi: 10.1161/01.hyp.10.5.497.

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