Extended tracts of homozygosity identify novel candidate genes associated with late-onset Alzheimer’s disease

M. A. Nalls; R. J. Guerreiro; J. Simon-Sanchez; J. T. Bras; B. J. Traynor; J. R. Gibbs; L. Launer; J. Hardy; A. B. Singleton

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Extended tracts of homozygosity identify novel candidate genes associated with late-onset Alzheimer’s disease

机译：延伸的纯合子鉴定出与迟发性阿尔茨海默氏病有关的新候选基因

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Large tracts of extended homozygosity are more prevalent in outbred populations than previously thought. With the advent of high-density genotyping platforms, regions of extended homozygosity can be accurately located allowing for the identification of rare recessive risk variants contributing to disease. We compared measures of extended homozygosity (greater than 1 Mb in length) in a population of 837 late-onset Alzheimer’s disease (LOAD) cases and 550 controls. In our analyses, we identify one homozygous region on chromosome 8 that is significantly associated with LOAD after adjusting for multiple testing. This region contains seven genes from which the most biologically plausible candidates are STAR, EIF4EBP1, and ADRB3. We also compared the total numbers of homozygous runs and the total length of these runs between cases and controls, showing a suggestive difference in these measures (p-values 0.052–0.062). This research suggests a recessive component to the etiology of LOAD.

机译：大范围延伸的纯合子在远亲群体中比以前认为的更为普遍。随着高密度基因分型平台的出现，扩展的纯合子区域可以被精确定位，从而可以识别出导致疾病的罕见隐性隐患。我们比较了837例迟发性阿尔茨海默氏病（LOAD）病例和550例对照人群中扩展的纯合性（长度大于1 Mb）的测量结果。在我们的分析中，我们经过多次测试调整后，在染色体8上确定了一个与LOAD显着相关的纯合区域。该区域包含七个基因，从生物学上看似最合理的候选基因是STAR，EIF4EBP1和ADRB3。我们还比较了病例和对照之间纯合子运行的总数和这些运行的总长度，显示了这些测量值的暗示性差异（p值0.052-0.062）。这项研究提示了LOAD病因的隐性组成部分。

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《neurogenetics》 |2009年第3期|183-190|共8页
作者
M. A. Nalls; R. J. Guerreiro; J. Simon-Sanchez; J. T. Bras; B. J. Traynor; J. R. Gibbs; L. Launer; J. Hardy; A. B. Singleton;
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Molecular Genetics Section and Laboratory of Neurogenetics National Institute on Aging National Institutes of Health Building 35 Room 1A1014 35 Convent Drive Bethesda MD 20892 USA;

Molecular Genetics Section and Laboratory of Neurogenetics National Institute on Aging National Institutes of Health Building 35 Room 1A1014 35 Convent Drive Bethesda MD 20892 USA;

Molecular Genetics Section and Laboratory of Neurogenetics National Institute on Aging National Institutes of Health Building 35 Room 1A1014 35 Convent Drive Bethesda MD 20892 USA;

Molecular Genetics Section and Laboratory of Neurogenetics National Institute on Aging National Institutes of Health Building 35 Room 1A1014 35 Convent Drive Bethesda MD 20892 USA;

Neurogenetics Branch National Institute of Neurological Disorders and Stroke National Institutes of Health Bethesda MD 20892 USA;

Molecular Genetics Section and Laboratory of Neurogenetics National Institute on Aging National Institutes of Health Building 35 Room 1A1014 35 Convent Drive Bethesda MD 20892 USA;

Laboratory of Epidemiology Demography and Biometry National Institute on Aging Bethesda MD 20892 USA;

Department of Molecular Neuroscience and Reta Lila Weston Institute of Neurological Studies Institute of Neurology University College London Queen Square London WC1N 3BG UK;

Molecular Genetics Section and Laboratory of Neurogenetics National Institute on Aging National Institutes of Health Building 35 Room 1A1014 35 Convent Drive Bethesda MD 20892 USA;

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正文语种 eng
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关键词
Alzheimer’s disease; Homozygous regions; APOE; Genetics;

机译：阿尔茨海默氏病;纯合区;APOE;遗传学;

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专利

1. Extended tracts of homozygosity identify novel candidate genes associated with late-onset Alzheimer's disease. [J] . Nalls MA, Guerreiro RJ, Simon Sanchez J Neurogenetics . 2009,第3期

机译：延伸的纯合子鉴定了与迟发性阿尔茨海默氏病相关的新候选基因。
2. Systems biology approach to late-onset Alzheimer's disease genome-wide association study identifies novel candidate genes validated using brain expression data and Caenorhabditis elegans experiments [J] . Shubhabrata Mukherjee, Joshua C. Russell, Daniel T. Carr, Alzheimer’s & dementia: the journal of the Alzheimer’s Association . 2017,第10期

机译：系统生物学方法是晚期疾病的疾病基因组 - 宽协会研究鉴定了使用脑表达数据和Caenorhabdise秀丽隐杆线虫实验验证的新型候选基因
3. A Bayesian Framework for Generalized Linear Mixed Modeling Identifies New Candidate Loci for Late-Onset Alzheimer’s Disease [J] . Xulong Wang, Vivek M. Philip, Guruprasad Ananda, Genetics: A Periodical Record of Investigations Bearing on Heredity and Variation . 2018,第1期

机译：广义线性混合建模的贝叶斯框架确定了晚期阿尔茨海默氏病的新候选基因座
4. Proteomics of Alzheimer's disease: Candidate proteins identified in serum as diagnostic biomarker for Alzheimer's disease [C] . Yu-Fen Lin, Ming-HuiYang, Yuan-Han Yang, American Society for Mass Spectrometry Conference on Mass Spectrometry and Allied Topics . 2012

机译：阿尔茨海默病的蛋白质组学：血清中鉴定的候选蛋白，作为阿尔茨海默病的诊断生物标志物
5. Investigation of genetic susceptibility to late-onset Alzheimer disease through genomic convergence. [D] . Liang, Xueying. 2007

机译：通过基因组收敛研究迟发性阿尔茨海默病的遗传易感性。
6. Extended tracts of homozygosity identify novel candidate genes associated with late onset Alzheimer’s Disease [O] . M. A. Nalls, R. J. Guerreiro, J. Simon-Sanchez, -1

机译：扩展的纯合子鉴定与晚期阿尔茨海默病相关的新型候选基因
7. Systems biology approach to late-onset Alzheimer's disease genome-wide association study identifies novel candidate genes validated using brain expression data and Caenorhabditis elegans experiments [O] . Shubhabrata Mukherjee, Joshua C. Russell, Daniel T. Carr, 2017

机译：系统生物学方法是晚期疾病的疾病基因组 - 宽协会研究鉴定了使用脑表达数据和Caenorhabdise Legans实验验证的新型候选基因

Extended tracts of homozygosity identify novel candidate genes associated with late-onset Alzheimer’s disease

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