Circulating Cell Free DNA and DNA Double-Strand Breakage in Alzheimer’s Disease

IF 2.8 Q2 NEUROSCIENCES
Michelle Nguyen, Colby Wood, Andres Rios, Zach Salter, P. H. Reddy
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引用次数: 0

Abstract

Alzheimer’s disease (AD) is an age-related neurodegenerative disease that is characterized by memory loss and multiple cognitive impairments. AD is pathologically characterized by age-dependent accumulation of amyloid-β protein and the phosphorylation of tau protein in the brains of patients with AD. Clinically, manifestations of AD include cognitive decline, dementia, alterations of high-order brain functions, and movement disorders. Double-stranded DNA breaks are a lethal form of DNA damage and are typically repaired via non-homologous end joining and homologous recombination. However, in AD brain, repair mechanism is disrupted, leading to a cascade of events, cognitive dysfunction, organ failure and reduced lifespan. Increased circulating cell-free DNA in the blood, cerebrospinal fluid, and urine in patients with AD, can be used as early detectable biomarkers for AD. The purpose of our article is to explore the potential uses of cell-free DNA and double-stranded DNA breaks as prognostic markers for AD and examine the recent research on the application of these markers in studies.
阿尔茨海默病中的循环细胞游离 DNA 和 DNA 双链断裂
阿尔茨海默病(AD)是一种与年龄相关的神经退行性疾病,以记忆力减退和多种认知障碍为特征。阿兹海默症的病理特征是阿兹海默症患者大脑中淀粉样蛋白-β的积累和tau蛋白的磷酸化。临床上,注意力缺失症的表现包括认知能力下降、痴呆、大脑高阶功能改变和运动障碍。双链DNA断裂是一种致命的DNA损伤形式,通常通过非同源末端连接和同源重组进行修复。然而,在注意力缺失症患者的大脑中,修复机制被破坏,导致一系列事件、认知功能障碍、器官衰竭和寿命缩短。AD患者血液、脑脊液和尿液中循环游离细胞DNA的增加可作为AD的早期生物标志物。本文旨在探讨无细胞DNA和双链DNA断裂作为AD预后标志物的潜在用途,并研究这些标志物在研究中的最新应用。
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CiteScore
2.80
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