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Neuropathological assessment and validation of mouse models for Alzheimer's disease: applying NIA-AA guidelines

机译:阿尔茨海默氏病小鼠模型的神经病理学评估和验证:应用NIA-AA指南

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Dozens of transgenic mouse models, generally based on mutations associated with familial Alzheimer's disease (AD), have been developed, in part, for preclinical testing of candidate AD therapies. However, none of these models has successfully predicted the clinical efficacy of drugs for treating AD patients. Therefore, development of more translationally relevant AD mouse models remains a critical unmet need in the field. A concept not previously implemented in AD preclinical drug testing is the use of mouse lines that have been validated for neuropathological features of human AD. Current thinking suggests that amyloid plaque and neurofibrillary tangle deposition is an essential component for accurate modeling of AD. Therefore, the AD translational paradigm would require pathologic Aβ and tau deposition, a disease-relevant distribution of plaques and tangles, and a pattern of disease progression of Aβ and tau isoforms similar to the neuropathological features found in the brains of AD patients. Additiona...
机译:已经开发了数十种通常基于与家族性阿尔茨海默氏病(AD)相关的突变的转基因小鼠模型,部分用于候选AD治疗的临床前测试。但是,这些模型均未成功预测药物治疗AD患者的临床疗效。因此,开发更多与翻译相关的AD鼠标模型仍然是该领域亟待解决的关键问题。 AD临床前药物测试以前未实现的概念是使用已针对人类AD的神经病理学特征进行验证的小鼠品系。当前的想法表明,淀粉样蛋白斑块和神经原纤维缠结是精确建模AD的重要组成部分。因此,AD翻译范例将需要病理性的Aβ和tau沉积,与疾病相关的斑块和缠结分布,以及Aβ和tau同工型的疾病进展模式,类似于AD患者大脑中的神经病理学特征。另外...

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