14 Alzheimer’s Disease: Genetics, Pathogenesis, Models, and Experimental Therapeutics

Cold Spring Harbor Monograph Archive Pub Date : 2008-01-01 DOI:10.1101/087969824.51.371

P. Wong, D. Price, L. Bertram, R. E. Tanzi

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引用次数: 1

Abstract

Alzheimer’s disease (AD), manifest as progressive loss of memory and cognitive impairments, affects more than 4 million individuals in the United States (Brookmeyer et al. 1998; Mayeux 2003; Cummings 2004; Wong et al. 2006). The index case, a middle-aged woman with behavioral disturbances and dementia, was described more than 100 years ago (Goedert and Spillantini 2006a; Hardy 2006a; Roberson and Mucke 2006; Small and Gandy 2006; Mandkelkow et al. 2007). Due to the postwar baby boom and increased life expectancy, the elderly are the most rapidly growing segment of our society and the number of persons with AD is predicted to triple over the next several decades. Prevalence, cost of care, impact on individuals and caregivers, and lack of mechanism-based treatments make AD one of the most challenging diseases of this new century (Price et al. 1998; Wong et al. 2002, 2006; Selkoe and Schenk 2003; Citron 2004a,b; Cummings 2004; Walsh and Selkoe 2004). This dementia syndrome results from dysfunction and death of neurons in specific brain regions/circuits, particularly those populations of neurons participating in memory and cognitive functions (Whitehouse et al. 1982; Hyman et al. 1984; Braak and Braak 1991, 1994; West et al. 1994, 2000, 2004; Price et al. 1998). The characteristic neuropathology of AD includes intracellular accumulations of phosphorylated Tau assembled in paired helical filaments (PHFs) within neurofibrillary tangles (NFTs) and abnormal neuritis, as well as extracellular Aβ peptide oligomers that, as aggregates, are at the core of neuritic amyloid plaques and represent sites of synaptic disconnection...

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阿尔茨海默病:遗传学、发病机制、模型和实验治疗

阿尔茨海默病(AD)表现为进行性记忆丧失和认知障碍，在美国影响了400多万人(Brookmeyer等人，1998;麦克斯2003;卡明斯2004;Wong et al. 2006)。索引病例是一位患有行为障碍和痴呆的中年妇女，早在100多年前就有记载(Goedert and Spillantini 2006a;哈迪2006;Roberson and Mucke 2006;Small and Gandy 2006;Mandkelkow et al. 2007)。由于战后婴儿潮和预期寿命的延长，老年人是我们社会中增长最快的部分，预计在未来几十年里，老年痴呆症患者的数量将增加两倍。患病率、护理费用、对个人和护理者的影响以及缺乏基于机制的治疗使阿尔茨海默病成为新世纪最具挑战性的疾病之一(Price et al. 1998;Wong et al. 2002, 2006;Selkoe and Schenk 2003;Citron 2004 a, b;卡明斯2004;Walsh and Selkoe 2004)。这种痴呆综合征是由特定脑区/回路的神经元功能障碍和死亡引起的，特别是那些参与记忆和认知功能的神经元群(Whitehouse et al. 1982;Hyman et al. 1984;Braak and Braak 1991,1994;West et al. 1994,2000,2004;Price et al. 1998)。阿尔茨海默病的特征性神经病理学包括在神经原纤维缠结(nft)内成对螺旋丝(PHFs)中组装的磷酸化Tau细胞内积聚和异常神经炎，以及作为聚集体的细胞外Aβ肽寡聚物，它们位于神经性淀粉样斑块的核心，代表突触断开的部位。

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Cold Spring Harbor Monograph Archive

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