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Viral-mediated gene delivery of constitutively activated G alpha s alters vasoreactivity.

机译:组成型激活的G alpha的病毒介导的基因传递改变了血管反应性。

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摘要

1. Decline in beta-adrenoceptor (beta-AR)-mediated function occurs with increasing age, as well as in multiple disease conditions. The mechanisms responsible for this decline include alterations in beta-AR itself, beta-AR coupling proteins, such as G-proteins, or other beta-AR-linked proteins, such as G-protein receptor kinases and/or phosphatases. 2. The present study examines the physiological effects of in vitro transfer of constitutively activated G alpha s (G alpha s-Q227L) to both cultured vascular smooth muscle cells (VSMC) and whole aortic tissue of 6-month-old (adult) animals via a replication-deficient Herpes simplex virus (HSV) vector. These studies were conducted to provide a model for future examination of the role of G alpha s in the age-related decline in beta-AR-mediated vasorelaxation. 3. Gene transfer was confirmed by western blotting for specific proteins. Aortic tissue infected with HSV-G alpha s-Q227L had reduced phenylephrine-induced contraction and enhanced isoproterenol-stimulated vasorelaxation. Infection of cultured VSMC with HSV-G alpha s-Q227L increased both basal- and isoproterenol-stimulated cAMP accumulation, whereas forskolin-stimulated cAMP production was unchanged. 4. These results implicate G alpha s as a target for further investigation in age-related changes in vascular reactivity and support the use of viral-mediated gene transfer as an effective tool to study adrenergic signal transduction and physiology in vascular tissue.
机译:1.随着年龄的增长以及多种疾病的发生,β-肾上腺素能受体(β-AR)介导的功能下降。造成这种下降的机制包括β-AR本身,β-AR偶联蛋白(例如G蛋白)或其他β-AR连接的蛋白(例如G蛋白受体激酶和/或磷酸酶)的改变。 2.本研究研究了将组成型激活的G alpha s(G alpha s-Q227L)体外转移到6个月大(成年)动物的培养的血管平滑肌细胞(VSMC)和整个主动脉组织中的生理作用通过复制缺陷型单纯疱疹病毒(HSV)载体。进行这些研究以提供模型,供将来检查Gα在年龄相关的β-AR介导的血管舒张下降中的作用。 3.通过蛋白质印迹的蛋白质印迹确认了基因转移。 HSV-Gαs-Q227L感染的主动脉组织减少了去氧肾上腺素引起的收缩,并增强了异丙肾上腺素刺激的血管舒张。 HSV-G alpha s-Q227L对培养的VSMC的感染增加了基础和异丙肾上腺素刺激的cAMP积累,而福司柯林刺激的cAMP产生却没有改变。 4.这些结果暗示G alpha s作为进一步研究与年龄相关的血管反应性变化的靶标,并支持使用病毒介导的基因转移作为研究血管组织中肾上腺素信号转导和生理学的有效工具。

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