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首页> 外文期刊>Brain pathology >Expression of cyclin-dependent kinase 5 mRNA and protein in the human brain following acute ischemic stroke.
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Expression of cyclin-dependent kinase 5 mRNA and protein in the human brain following acute ischemic stroke.

机译:急性缺血性中风后人脑中细胞周期蛋白依赖性激酶5 mRNA和蛋白的表达。

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Neuronal cell death after brain ischemia may be regulated by activation of cyclin-dependent kinase 5 (Cdk5). In this study, expression of Cdk5 and its activator p35/p25 was examined in human post-mortem stroke tissue and in human cerebral cortical fetal neurons and human brain microvascular endothelial cells exposed to oxygen-glucose deficiency and reperfusion. The majority of patients demonstrated increased expression of Cdk5 and p-Cdk5 in stroke-affected tissue, with about a third showing increased p35 and p25 cleaved fragment as determined by Western blotting. An increase in Cdk5-, p-Cdk5- and p35-positive neurons and microvessels occurred in stroke-affected regions of patients. Staining of neurons became irregular and clumped in the cytoplasm, and nuclear translocation occurred, with colocalization of p35 and Cdk5. Association of Cdk5 with nuclear damage was demonstrated by coexpression of nuclear Cdk5 in TUNEL-positive neurons and microvessels in peri-infarcted regions. In vitro studies showed up-regulation and/or nuclear translocation of Cdk5, p-Cdk5 and p35 in neurons and endothelial cells subjected to oxygen-glucose deficiency, and strong staining was associated with propidium iodide positive nuclei, an indicator of cellular damage. These results provide new evidence for a role of Cdk5 in the events associated with response to ischemic injury in humans.
机译:脑缺血后神经元细胞的死亡可通过细胞周期蛋白依赖性激酶5(Cdk5)的激活来调节。在这项研究中,Cdk5及其激活剂p35 / p25在人死后中风组织以及暴露于氧-葡萄糖缺乏和再灌注的人大脑皮质胎儿神经元和人脑微血管内皮细胞中进行了检测。大多数患者表现出在受中风影响的组织中Cdk5和p-Cdk5的表达增加,而大约三分之一的患者通过Western blot检测显示p35和p25裂解的片段增加。在患者的中风影响区域中,Cdk5-,p-Cdk5-和p35阳性神经元和微血管增加。神经元的染色变得不规则并聚集在细胞质中,并且发生核易位,与p35和Cdk5共定位。 TUNEL阳性神经元和梗死周围区域的微血管共表达核Cdk5,证明了Cdk5与核损伤的相关性。体外研究表明,遭受氧葡萄糖缺乏的神经元和内皮细胞中Cdk5,p-Cdk5和p35的上调和/或核易位,并且强染色与碘化丙锭阳性核有关,后者是细胞损伤的指标。这些结果为Cdk5在与人类对缺血性损伤的反应相关的事件中的作用提供了新的证据。

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