An overview of the genes and biomarkers in Alzheimer's disease.

Hari Krishnan Krishnamurthy, Vasanth Jayaraman, Karthik Krishna, Tianhao Wang, Kang Bei, Chithra Changalath, John J Rajasekaran
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Abstract

Alzheimer's disease (AD) is the most common type of dementia and neurodegenerative disease characterized by neurofibrillary tangles (NFTs) and amyloid plaque. Familial AD is caused by mutations in the APP, PSEN1, and PSEN2 genes and these mutations result in the early onset of the disease. Sporadic AD usually affects older adults over the age of 65 years and is, therefore classified as late-onset AD (LOAD). Several risk factors associated with LOAD including the APOE gene have been identified. Moreover, GWAS studies have identified a wide array of genes and polymorphisms that are associated with LOAD risk. Currently, the diagnosis of AD involves the evaluation of memory and personality changes, cognitive impairment, and medical and family history to rule out other diseases. Laboratory tests to assess the biomarkers in the body fluids as well as MRI, CT, and PET scans to analyze the presence of plaques and NFTs are also included in the diagnosis of AD. It is important to diagnose AD before the onset of clinical symptoms, i.e. during the preclinical stage, to delay the progression and for better management of the disease. Research has been conducted to identify biomarkers of AD in the CSF, serum, saliva, and urine during the preclinical stage. Current research has identified several biomarkers and potential biomarkers in the body fluids that enhance diagnostic accuracy. Aside from genetics, other factors such as diet, physical activity, and lifestyle factors may influence the risk of developing AD. Clinical trials are underway to find potential biomarkers, diagnostic measures, and treatments for AD mainly in the preclinical stage. This review provides an overview of the genes and biomarkers of AD.

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阿尔茨海默病的基因和生物标志物综述。
阿尔茨海默病(AD)是最常见的痴呆症和神经退行性疾病,其特征是神经原纤维缠结(nft)和淀粉样斑块。家族性AD是由APP、PSEN1和PSEN2基因突变引起的,这些突变导致疾病的早期发病。散发性阿尔茨海默病通常发生在65岁以上的老年人身上,因此被归类为迟发性阿尔茨海默病(LOAD)。包括APOE基因在内的几个与LOAD相关的危险因素已经被确定。此外,GWAS研究已经确定了与LOAD风险相关的一系列基因和多态性。目前,AD的诊断包括评估记忆和人格改变、认知障碍、病史和家族史,以排除其他疾病。用于评估体液中生物标志物的实验室测试以及用于分析斑块和nft存在的MRI、CT和PET扫描也包括在AD的诊断中。重要的是在临床症状出现之前,即在临床前阶段诊断阿尔茨海默病,以延缓病情进展并更好地控制疾病。在临床前阶段,已经进行了研究,以确定脑脊液、血清、唾液和尿液中的AD生物标志物。目前的研究已经确定了体液中的几种生物标志物和潜在生物标志物,可以提高诊断的准确性。除遗传因素外,饮食、体育活动和生活方式等因素也可能影响患AD的风险。临床试验正在进行中,主要是在临床前阶段寻找潜在的生物标志物、诊断措施和治疗方法。本文综述了阿尔茨海默病的基因和生物标志物。
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