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短暂性前脑缺血后c-fos和fos-B蛋白的表达:低温的影响

Expression of c-fos and fos-B proteins following transient forebrain ischemia: effect of hypothermia.

作者信息

Kumar K, Wu X, Evans A T

机构信息

Department of Pathology, Michigan State University, East Lansing 48824, USA.

出版信息

Brain Res Mol Brain Res. 1996 Dec;42(2):337-43. doi: 10.1016/s0169-328x(96)00181-7.

Abstract

Immediate early genes are induced by transient global ischemia. Using immunohistochemistry we studied the effect of intraischemic hypothermia (30 degrees C) on the expression of c-fos and fos-B proteins following 10 min forebrain ischemia in the gerbil. Postischemia (PI) periods of 1 hour (h), 6 h, 1 day (d) and 2 d and nonischemic controls were examined in normothermic and hypothermic brains. In normothermic ischemic brains, marked expression of c-fos occurred in the dentate gyrus after 1 h PI which extended to CA2-4 regions by 6 h. Hypothermia hastened the time course of c-fos expression as it was expressed simultaneously in the dentate gyrus as well as CA2-4 regions after only 1 h, and by 6 h the expression remained only in the CA2-4 regions and not the dentate gyrus in hypothermic ischemic brains. There was no difference in its expression between normothermic and hypothermic brains in the 1 d and 2 d PI animals. Somewhat similar changes were noted in fos-B expression. In normothermic ischemic brains fos-B was induced in the dentate gyrus by 1 h PI, and by 6 h it extended to involve CA1-4 cells. The hypothermic ischemic brains showed faster induction of fos-B so that the dentate gyrus as well as CA1-4 regions were immunopositive at 1 h PI. There was no difference in its expression between normothermic and hypothermic brains in the subsequent PI periods of 6 h, 1 d and 2 d. The shift towards faster sequential induction of these genes by hypothermia in ischemic brains may be indicative of preservation of or faster recovery of mechanisms involved in intracellular signalling.

摘要

即刻早期基因由短暂性全脑缺血诱导产生。我们采用免疫组织化学方法,研究了在沙土鼠前脑缺血10分钟后,缺血期低温(30摄氏度)对c-fos和Fos-B蛋白表达的影响。对体温正常和低温状态下的大脑,分别检测了缺血后1小时(h)、6小时、1天(d)和2天的情况以及非缺血对照组。在体温正常的缺血大脑中,缺血后1小时齿状回出现明显的c-fos表达,6小时时扩展至CA2-4区。低温加速了c-fos的表达进程,因为仅1小时后齿状回以及CA2-4区就同时出现了表达,而在低温缺血大脑中,6小时时表达仅保留在CA2-4区,齿状回中已无表达。在缺血后1天和2天的动物中,体温正常和低温大脑中其表达无差异。Fos-B表达也有类似变化。在体温正常的缺血大脑中,缺血后1小时Fos-B在齿状回中被诱导表达,6小时时扩展至CA1-4细胞。低温缺血大脑中Fos-B的诱导更快,因此在缺血后1小时齿状回以及CA1-4区免疫反应均呈阳性。在随后的缺血后6小时、1天和2天,体温正常和低温大脑中其表达无差异。低温使缺血大脑中这些基因更快地依次诱导表达,这可能表明细胞内信号传导相关机制得到了保留或恢复得更快。

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