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G蛋白在实验性内膜增生中的表达及功能

The expression and function of G-proteins in experimental intimal hyperplasia.

作者信息

Davies M G, Ramkumar V, Gettys T W, Hagen P O

机构信息

Department of Surgery, Duke University Medical Center, Durham, North Carolina 27710.

出版信息

J Clin Invest. 1994 Oct;94(4):1680-9. doi: 10.1172/JCI117513.

Abstract

G-proteins are membrane-bound signal transduction proteins which couple extracellular receptor signals to various effectors. This study examines the expression and the function of G-proteins (alpha i, alpha s, alpha q, and alpha o) in experimental intimal hyperplasia. Vein bypass grafts were placed in 30 New Zealand White rabbits and were harvested after 28 d. The contralateral jugular veins served as controls. Isometric tension studies were performed on rings from veins and vein grafts (n = 10), and Western blot and mRNA analyses were performed in another 20 vessels. There was a fivefold increase in alpha q, a 2.7-fold increase in the alpha i2, and a 3.3-fold increase in alpha s expressions in vein grafts compared with veins. Detectable expression of alpha i3 was observed in vein grafts but not in jugular veins. In addition, there was a 3.8-fold increase in beta subunits in the vein grafts compared with the veins. mRNA for alpha s, alpha i3, and alpha i2 were all elevated in the vein grafts. No detectable levels of the alpha i1 protein or its mRNA were present in either veins or vein grafts. Contractile responses in the veins were not inhibited by pertussis toxin. The contractile responses to norepinephrine were enhanced by twofold, and the responses to serotonin developed de novo in vein grafts compared with veins. The contractile responses to both norepinephrine and serotonin were only partially inhibited by pertussis toxin in the vein grafts even though there was 100% ADP ribosylation with pertussis toxin in both veins and vein grafts. These data suggest that intimal hyperplasia is associated with increased or novel expression of G-proteins in vivo which occur simultaneously with the development of pertussis toxin-sensitive contractile responses. Changes in G-proteins at a transcriptional level or at the level of RNA stability may be involved in the response of smooth muscle cells to injury and to intimal hyperplasia formation.

摘要

G蛋白是膜结合信号转导蛋白,可将细胞外受体信号与各种效应器偶联。本研究检测了G蛋白(αi、αs、αq和αo)在实验性内膜增生中的表达及功能。将静脉旁路移植物植入30只新西兰白兔体内,28天后取出。对侧颈静脉作为对照。对静脉和静脉移植物的血管环进行等长张力研究(n = 10),并对另外20个血管进行蛋白质印迹和mRNA分析。与静脉相比,静脉移植物中αq增加了5倍,αi2增加了2.7倍,αs表达增加了3.3倍。在静脉移植物中观察到αi3有可检测到的表达,但颈静脉中未观察到。此外,与静脉相比,静脉移植物中的β亚基增加了3.8倍。静脉移植物中αs、αi3和αi2的mRNA均升高。静脉和静脉移植物中均未检测到αi1蛋白或其mRNA的水平。静脉中的收缩反应不受百日咳毒素抑制。与静脉相比,静脉移植物中对去甲肾上腺素的收缩反应增强了两倍,对5-羟色胺的反应是新出现的。即使静脉和静脉移植物中百日咳毒素的ADP核糖基化均为100%,静脉移植物中对去甲肾上腺素和5-羟色胺的收缩反应仅被百日咳毒素部分抑制。这些数据表明,内膜增生与体内G蛋白表达增加或新表达有关,这些变化与百日咳毒素敏感的收缩反应的发展同时发生。G蛋白在转录水平或RNA稳定性水平的变化可能参与平滑肌细胞对损伤和内膜增生形成的反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9323/295331/4222d732fa3a/jcinvest00022-0341-a.jpg

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