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高血压患者中 GRK2 表达增强和βAR 血管舒张的脱敏作用。

Enhanced GRK2 expression and desensitization of betaAR vasodilatation in hypertensive patients.

机构信息

Dipartimento di Medicina Clinica Scienze Cardiovascolari ed Immunologiche, Federico II University of Naples, Italy.

出版信息

Clin Transl Sci. 2008 Dec;1(3):215-20. doi: 10.1111/j.1752-8062.2008.00050.x.

Abstract

Increased levels of G protein coupled receptor kinase GRK2 appear to participate in hypertension presumably through the desensitization of beta adrenergic receptors (betaARs) that mediate vasodilatation. There are contrasting data on the occurrence of betaAR desensitization in the vasculature, we therefore investigated betaAR vasodilatation and desensitization in normotensives and in hypertensive humans. In blood lymphocytes, we assessed betaAR signaling and GRK2 expression and found betaAR signaling alterations and, consistent with desensitization, ncreased GRK2 levels in hypertensives. We studied in vivo vasodilatation to the betaAR agonist isoproterenol (ISO) injected in the brachia artery in control conditions and during the concomitant infusion of heparin, a known in vitro nonspecific GRK inhibitor. ISO induced a dose-dependent vasorelaxation that was attenuated in hypertensives indicating a loss of betaAR signaling. Intra-arterial infusion of heparin nhibited lymphocyte GRK2 activity and prevented desensitization of betaAR vasodilatation in normotensives. In hypertensives, heparin restored vasodilatation to ISO, to levels observed in normotensives. Our results suggest that betaAR desensitization does indeed occur at the vascular levels in vivo, and that heparin by acting as a GRK inhibitor prevents this in normotensives and restores impaired betaAR vasodilation in hypertensives. We conclude that desensitization participates to impaired betaAR vasodilation in hypertension.

摘要

G 蛋白偶联受体激酶 2(GRK2)水平升高似乎参与了高血压的发生,可能是通过β肾上腺素能受体(βAR)脱敏来介导血管舒张。关于血管中βAR 脱敏的发生存在相互矛盾的数据,因此我们研究了正常人和高血压患者的βAR 血管舒张和脱敏。在血液淋巴细胞中,我们评估了βAR 信号和 GRK2 表达,发现高血压患者存在βAR 信号改变,并且与脱敏一致,GRK2 水平升高。我们研究了在控制条件下和同时输注肝素(一种已知的体外非特异性 GRK 抑制剂)时,βAR 激动剂异丙肾上腺素(ISO)注射到肱动脉中引起的体内血管舒张。ISO 诱导剂量依赖性血管舒张,在高血压患者中减弱,表明βAR 信号丢失。动脉内输注肝素抑制淋巴细胞 GRK2 活性并防止正常血压者的βAR 血管舒张脱敏。在高血压患者中,肝素将 ISO 引起的血管舒张恢复至正常血压者观察到的水平。我们的结果表明,βAR 脱敏确实在体内血管水平发生,肝素通过作为 GRK 抑制剂起作用,可防止正常血压者发生这种情况,并恢复高血压者受损的βAR 血管舒张。我们得出结论,脱敏参与了高血压中受损的βAR 血管舒张。

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