首页> 外文期刊>Progress in Neuro-Psychopharmacology & Biological Psychiatry: An International Research, Review and News Journal >DNA damage and apoptosis in the aged canine brain: relationship to Abeta deposition in the absence of neuritic pathology.
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DNA damage and apoptosis in the aged canine brain: relationship to Abeta deposition in the absence of neuritic pathology.

机译:老年犬脑中的DNA损伤和凋亡:在缺乏神经病理学的情况下与Abeta沉积的关系。

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摘要

1. In addition to beta-amyloid (Abeta) deposition and cytoskeletal neuropathology, both the Alzheimer's disease (AD) and Down's syndrome (DS) human brain exhibit marked evidence of DNA damage, however, it is difficult to separate events that occur in conjunction with neurofibrillary pathology versus Abeta pathology in these systems. 2. In contrast, the aged canine brain exhibits the accumulation of Abeta into diffuse deposits similar to those found in early AD and DS in the absence of neurofibrillary pathology. Furthermore, Abeta deposition in canine brain is correlated with cognitive deficits. 3. In order to test the hypothesis that TUNEL labeling for DNA damage in AD is not simply a consequence of agonal artifacts, postmortem artifacts, or neurofibrillary pathology, and may be directly related to Abeta deposition, we examined Abeta immunoreactivity, PHF-1 immunoreactivity, and TUNEL labeling in this animal model. 4. These experiments reveal a relationship between the amount of DNA damage detected by TUNEL labeling and levels of Abeta deposition. Further, in animals with no TUNEL labeling, we detected no Abeta immunoreactivity. 5. These data support the hypothesis that TUNEL labeling in AD ans DS is not a consequence of agonal artifact, postmortem artifact, or tau pathology, and may be directly related to Abeta deposition and perhaps AD pathogenesis.
机译:1.除β淀粉样蛋白(Abeta)沉积和细胞骨架神经病理学外,人脑的阿尔茨海默氏病(AD)和唐氏综合症(DS)均显示出DNA损伤的明显证据,但是,很难分离出一起发生的事件这些系统中神经原纤维病理与Abeta病理的关系。 2.相反,在没有神经原纤维病理的情况下,老年犬脑表现出Abeta积累成弥漫性沉积物的现象,类似于早期AD和DS中发现的情况。此外,犬脑中的Abeta沉积与认知缺陷有关。 3.为了检验假说TUNEL标记AD中的DNA损伤不仅是神经假象,验尸假象或神经原纤维病理学的结果,而且可能与Abeta沉积直接相关,我们检查了Abeta免疫反应性,PHF-1免疫反应性,以及该动物模型中的TUNEL标记。 4.这些实验揭示了通过TUNEL标记检测到的DNA损伤量与Abeta沉积水平之间的关系。此外,在没有TUNEL标记的动物中,我们没有检测到Abeta免疫反应性。 5.这些数据支持以下假设,即AD ans DS中的TUNEL标记不是痛苦的假象,验尸假象或tau病理学的结果,并且可能与Abeta沉积以及AD的发病机理直接相关。

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