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未来患酒精成瘾症风险高低不同的男性中鸟苷三磷酸结合蛋白的差异表达

Differential expression of guanosine triphosphate binding proteins in men at high and low risk for the future development of alcoholism.

作者信息

Wand G S, Waltman C, Martin C S, McCaul M E, Levine M A, Wolfgang D

机构信息

Department of Medicine, Johns Hopkins University School of Medicine, Baltimore, Maryland 21205.

出版信息

J Clin Invest. 1994 Sep;94(3):1004-11. doi: 10.1172/JCI117413.

Abstract

We evaluated G-proteins that are components of adenylyl cyclase (AC) signal transduction in erythrocyte and lymphocyte membranes from 26 family history positive (FHP) non-alcoholic and 26 family history negative (FHN) nonalcoholic subjects. Subjects were classified as FHP if their father met criteria for alcohol dependence; as FHN, if there was no history of alcoholism in any first or second degree relatives. Immunoblot analysis indicated that levels of erythrocyte membrane Gs alpha from FHP subjects were greater than levels in FHN subjects (171 +/- 11 vs 100 +/- 6, P < 0.001). To confirm the results of the immunoblot analysis, Gs alpha was quantitated by cholera toxin-dependent [32P]ADP-ribosylation. Levels of erythrocyte [32P]ADP-ribose-Gs alpha from FHP subjects were greater than levels in FHN subjects (236 +/- 28 vs 100 +/- 14, P < 0.001). Gs alpha levels did not correlate with age or alcohol consumption. By contrast to differences in Gs alpha, immunoblot analysis showed similar levels of Gi(2)alpha and Gi(3)alpha in erythrocyte membranes of FHP and FHN subjects. Pertussis toxin-catalyzed [32P]ADP-ribosylation of Gi-like G-proteins confirmed the immunoblot observations. Lastly, compared to FHN subjects, FHP subjects had enhanced Gs alpha expression in lymphocyte membranes as well (138 +/- 11 vs 100 +/- 5.5; P < 0.02). In summary, compared to FHN nonalcoholic men, FHP nonalcoholic men had greater levels of the stimulatory G-protein, Gs alpha, in erythrocyte and lymphocyte membranes. Enhanced expression of Gs alpha may be a marker of increased risk for the future development of alcoholism.

摘要

我们评估了26名家族史阳性(FHP)非酒精性受试者和26名家族史阴性(FHN)非酒精性受试者红细胞膜和淋巴细胞膜中作为腺苷酸环化酶(AC)信号转导成分的G蛋白。如果受试者的父亲符合酒精依赖标准,则将其分类为FHP;如果其任何一级或二级亲属均无酗酒史,则分类为FHN。免疫印迹分析表明,FHP受试者红细胞膜Gsα水平高于FHN受试者(171±11对100±6,P<0.001)。为了证实免疫印迹分析结果,通过霍乱毒素依赖性[32P]ADP-核糖基化对Gsα进行定量。FHP受试者红细胞[32P]ADP-核糖-Gsα水平高于FHN受试者(236±28对100±14,P<0.001)。Gsα水平与年龄或饮酒量无关。与Gsα的差异形成对比的是,免疫印迹分析显示FHP和FHN受试者红细胞膜中Gi(2)α和Gi(3)α水平相似。百日咳毒素催化的Gi样G蛋白的[32P]ADP-核糖基化证实了免疫印迹观察结果。最后,与FHN受试者相比,FHP受试者淋巴细胞膜中Gsα表达也增强(138±11对100±5.5;P<0.02)。总之,与FHN非酒精性男性相比,FHP非酒精性男性红细胞膜和淋巴细胞膜中刺激性G蛋白Gsα水平更高。Gsα表达增强可能是未来发生酒精中毒风险增加的一个标志。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1fea/295148/a4c004ca3ff6/jcinvest00021-0104-a.jpg

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