首页> 外文期刊>Neuropathology and applied neurobiology >Neuropil and neuronal changes in hippocampal NADPH-diaphorase histochemistry in the ME7 model of murine prion disease.
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Neuropil and neuronal changes in hippocampal NADPH-diaphorase histochemistry in the ME7 model of murine prion disease.

机译:小鼠病毒病ME7模型中海马NADPH-心肌黄递酶组织化学的神经纤维和神经元变化。

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Nitric oxide (NO) has been implicated in neurotoxicity and cerebral blood flow changes in chronic neurodegeneration, but its activity in the mammalian prion diseases has not been studied in detail. Nicotine adenine dinucleotide phosphate (NADPH)-diaphorase (NADPH-d) histochemistry is a simple and robust histochemical procedure that allows localization of the tissue distribution of NO synthases. The aim of the present study is to assess whether NADPH-d histochemical activity is altered in the hippocampus in the ME7 model of prion disease in C57BL/6J mice. At early and late stages after the initiation of the disease we assessed features of the NADPH-d positive cells and the neuropil histochemical activity in CA1 and dentate gyrus using densitometric analysis. In C57BL/6J mice 13 weeks postinjection of the prion agent ME7, when behavioural changes first become apparent, neuropil NADPH-d histochemical staining increases, whereas at late stages it decreases dramatically. Both type I and type II NADPH-d positive cells were found to survive throughout the hippocampal formation into the late stages of the disease, but diaphorase activity was reduced in dendritic branches and abnormal varicosities were present in both dendritic and axonal processes of NADPH-d positive type I cells. The pathophysiological implications of the results remain to be investigated but both blood flow alteration and NO neurotoxicity may be features of the disease.
机译:一氧化氮(NO)与慢性神经退行性病变的神经毒性和脑血流变化有关,但尚未详细研究其在哺乳动物pr病毒疾病中的活性。尼古丁腺嘌呤二核苷酸磷酸(NADPH)-心肌黄酶(NADPH-d)的组织化学是一种简单而强大的组织化学程序,可用于定位NO合酶的组织分布。本研究的目的是评估在C57BL / 6J小鼠的ion病毒病ME7模型中,海马中NADPH-d的组织化学活性是否改变。在疾病发生后的早期和晚期,我们使用光密度分析法评估了CA1和齿状回中NADPH-d阳性细胞的特征以及神经纤维组织化学活性。在注射57病毒剂ME7后13周的C57BL / 6J小鼠中,当行为变化首先变得明显时,neuropil NADPH-d组织化学染色增加,而在后期阶段,其显着降低。发现I型和II型NADPH-d阳性细胞在整个海马形成期间一直存活到疾病晚期,但是树突状分支中的黄递酶活性降低,NADPH-d的树突状和轴突过程均存在异常的静脉曲张。阳性I型细胞。结果的病理生理影响尚待研究,但血流改变和NO神经毒性均可能是该疾病的特征。

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