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大鼠脑局灶性缺血后热休克蛋白-70 mRNA和c-fos mRNA的区域表达

Regional expression of heat shock protein-70 mRNA and c-fos mRNA following focal ischemia in rat brain.

作者信息

Welsh F A, Moyer D J, Harris V A

机构信息

Division of Neurosurgery, University of Pennsylvania School of Medicine, Philadelphia.

出版信息

J Cereb Blood Flow Metab. 1992 Mar;12(2):204-12. doi: 10.1038/jcbfm.1992.30.

Abstract

In situ hybridization was used to estimate regional levels of heat shock protein-70 (HSP-70) mRNA and c-fos mRNA in two related models of focal cerebral ischemia. In the first model, permanent occlusion of the distal middle cerebral artery (MCA) alone caused a patchy increase in HSP-70 mRNA by 1 h in the central zone of the MCA territory of the ipsilateral neocortex. Tissue levels of HSP-70 mRNA continued to increase for several hours and remained elevated at 24 h. In contrast to the focal expression of HSP-70, c-fos mRNA was increased throughout the ipsilateral cerebral cortex by 15 min and remained elevated for least 3 h. The wide distribution of c-fos expression suggests it may have been caused by spreading depression. In the second model, severe focal ischemia was produced with a combination of transient (1-h) bilateral carotid artery occlusion and permanent MCA occlusion. Combined occlusion for 1 h without reperfusion caused expression of HSP-70 mRNA only in regions adjacent to the central zone of the MCA territory of the neocortex. However, reperfusion of the carotids for 2 h generated intense expression of HSP-70 mRNA throughout most of the ipsilateral cerebral cortex, white matter, striatum, and hippocampus. The wide-spread increase in HSP-70 mRNA suggests that reperfusion triggered expression in all previously ischemic regions. However, at 24 h of reperfusion, increased levels of HSP-70 mRNA were restricted primarily to the ischemic core of the neocortex. These results suggest that expression of HSP-70 mRNA is prolonged in regions undergoing injury, but is transient in surrounding regions that recover.

摘要

原位杂交技术用于评估局灶性脑缺血两个相关模型中热休克蛋白70(HSP - 70)mRNA和c - fos mRNA的区域水平。在第一个模型中,单纯永久性阻断大脑中动脉(MCA)远端,可在1小时内使同侧新皮质MCA区域中心区的HSP - 70 mRNA呈斑片状增加。HSP - 70 mRNA的组织水平持续升高数小时,并在24小时时仍保持升高。与HSP - 70的局灶性表达不同,c - fos mRNA在同侧大脑皮质中15分钟内即增加,并至少持续升高3小时。c - fos表达的广泛分布表明其可能由扩散性抑制引起。在第二个模型中,通过短暂(1小时)双侧颈动脉阻断和永久性MCA阻断相结合产生严重局灶性缺血。联合阻断1小时且无再灌注仅导致新皮质MCA区域中心区相邻区域的HSP - 70 mRNA表达。然而,颈动脉再灌注2小时后,同侧大部分大脑皮质、白质、纹状体和海马中均出现HSP - 70 mRNA的强烈表达。HSP - 70 mRNA的广泛增加表明再灌注触发了所有先前缺血区域的表达。然而,在再灌注24小时时,HSP - 70 mRNA水平升高主要局限于新皮质的缺血核心区。这些结果表明,HSP - 70 mRNA在受损区域的表达持续时间延长,但在恢复的周围区域是短暂的。

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