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首页> 外文期刊>Pathology Research and Practice >Use of 2,3,5-triphenyltetrazolium chloride-stained brain tissues for immunofluorescence analyses after focal cerebral ischemia in rats
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Use of 2,3,5-triphenyltetrazolium chloride-stained brain tissues for immunofluorescence analyses after focal cerebral ischemia in rats

机译:在大鼠局灶性脑缺血后,使用2,3,5-三苯基四唑氯化物染色脑组织进行免疫荧光分析

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摘要

The middle cerebral artery occlusion (MCAO) model in rodents has been widely used as model for studying brain ischemic stroke. TTC (2,3,5-triphenyltetrazolium chloride) staining in fresh tissues is used to evaluate the size of the infarct in MCAO model, and TTC-stained brain tissues are considered to be possible to bring a damage to the anatomical structure of neuronal cells and unsuitable for immunofluorescence analyses of cytology, and discarded after evaluation of infarct volume. Another group of models with in vivo fixation was required to the pathological or histological analyses of the infarct brains, which lead to double the numbers of animals in researches. However, some evidences indicate that if we properly optimized staining protocol, TTC-stained brain tissues might be suitable for cytological analyses. In this work, we have optimized the immunofluorescent staining methods of TTC-stained brain slices, and found that TTC-stained brain tissues are suitable for quantitative and qualitative analyses of microglia, astrocytes and neuroblasts, the morphology of theses cell were nearly identical to the in-vivo fixed models. Our optimized-protocol provide two advantages over traditional methods one of them is providing the precise the infarct region, which reduces the differences within groups, the other one is decreasing the total number of animals in research dramatically.
机译:啮齿动物中的中脑动脉闭塞(MCAO)模型被广泛用作学习脑缺血性卒中的模型。在新鲜组织中染色的TTC(2,3,5-三苯基四氯化氢氯化铵)用于评估MCAO模型中梗塞的尺寸,并且认为TTC染色的脑组织可以损坏神经元细胞的解剖结构并且不适用于细胞学的免疫荧光分析,并在评估梗塞体积后丢弃。对梗死脑的病理或组织学分析需要另一组用于体内固定的模型,这导致研究中的动物的数量增加了两倍。然而,一些证据表明,如果我们正确优化染色方案,TTC染色的脑组织可能适合细胞学分析。在这项工作中,我们优化了TTC染色的脑切片的免疫荧光染色方法,发现TTC染色的脑组织适用于微胶质细胞,星形细胞和神经细胞的定量和定性分析,蛋白质的形态几乎与之相同体内固定模型。我们的优化协议提供了两种优势,它与传统方法相比,其中一个是提供精确的梗塞区域,这减少了群体内的差异,另一个是急剧下降研究中的动物总数。

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