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双相情感障碍中G蛋白α(s)亚基和α(i2)亚基mRNA表达异常。

Abnormal G protein alpha(s) - and alpha(i2)-subunit mRNA expression in bipolar affective disorder.

作者信息

Spleiss O, van Calker D, Schärer L, Adamovic K, Berger M, Gebicke-Haerter P J

机构信息

Department of Biology II, University of Freiburg, Freiburg i Br, Germany.

出版信息

Mol Psychiatry. 1998 Nov;3(6):512-20. doi: 10.1038/sj.mp.4000393.

Abstract

Disturbances of events associated with intracellular signaling pathways have been suspected of involvement in the development or progression of affective disorders. Often, heterotrimeric G proteins are located at the beginning of these pathways as modulators of extracellular messages. For this reason, messenger RNA expression of three G protein alpha-subunits and of phosphatidylinositol-3 kinase (PI-3 K) regulatory subunit p85 was examined in granulocytes from patients with bipolar or unipolar affective disorder and compared to healthy controls. Messenger RNA expression of the G protein subunit alpha(q) and of p85 was identical in unipolar and bipolar patients and in controls. Furthermore, mRNAs of G protein subunits alpha(s) and alpha(i2) were not different in unipolar patients as compared to healthy controls. Alpha(s) mRNA, however, was markedly increased in bipolar patients. This increase was observed in lithium-treated (more than 12 months) and in unmedicated patients. Elevated levels of alpha(i2) mRNA in unmedicated bipolar patients did not reach statistical significance, whereas mRNA in bipolar patients receiving lithium was significantly above controls. Finally, long-term medication of unipolar patients with lithium had no influence on alpha(i2) mRNA levels. The data reveal elevated mRNA levels of G alpha(s) as a robust feature of bipolar affective disorder. Moreover, despite responsiveness of alpha(i2) gene expression to cAMP-related events, no substantial upregulation of alpha(i2) mRNA was observed in bipolar patients. The lack of alpha(i2) mRNA upregulation, hence, could be an additional abnormality in these patients. Even though lithium was able to reinstate this upregulation, there was no feedback downregulation of alpha(s). This strongly supports the notion of major disturbances of the cAMP signaling system in bipolar illness.

摘要

细胞内信号通路相关事件的紊乱被怀疑与情感障碍的发生或进展有关。通常,异源三聚体G蛋白作为细胞外信息的调节因子位于这些信号通路的起始位置。因此,研究了双相或单相情感障碍患者粒细胞中三种G蛋白α亚基和磷脂酰肌醇-3激酶(PI-3K)调节亚基p85的信使核糖核酸(mRNA)表达,并与健康对照进行比较。G蛋白亚基α(q)和p85的mRNA表达在单相和双相患者以及对照中是相同的。此外,与健康对照相比,单相患者中G蛋白亚基α(s)和α(i2)的mRNA没有差异。然而,双相患者中α(s) mRNA明显增加。在接受锂治疗(超过12个月)的患者和未用药的患者中均观察到这种增加。未用药的双相患者中α(i2) mRNA水平升高未达到统计学意义,而接受锂治疗的双相患者的mRNA显著高于对照。最后,单相患者长期使用锂治疗对α(i2) mRNA水平没有影响。数据显示Gα(s) mRNA水平升高是双相情感障碍的一个显著特征。此外,尽管α(i2)基因表达对与环磷酸腺苷(cAMP)相关的事件有反应,但在双相患者中未观察到α(i2) mRNA的实质性上调。因此,α(i2) mRNA上调的缺乏可能是这些患者的另一种异常情况。尽管锂能够恢复这种上调,但α(s)并没有反馈下调。这有力地支持了双相情感障碍中cAMP信号系统存在重大紊乱的观点。

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