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Screening and Evaluation of Deleterious SNPs in APOE Gene of Alzheimer’s Disease

机译:阿尔茨海默病APOE基因中有害SNPs的筛选和评价

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Introduction. Apolipoprotein E (APOE) is an important risk factor for Alzheimer’s disease (AD) and is present in 30–50% of patients who develop late-onset AD. Several single-nucleotide polymorphisms (SNPs) are present in APOE gene which act as the biomarkers for exploring the genetic basis of this disease. The objective of this study is to identify deleterious nsSNPs associated with APOE gene.Methods. The SNPs were retrieved from dbSNP. Using I-Mutant, protein stability change was calculated. The potentially functional nonsynonymous (ns) SNPs and their effect on protein was predicted by PolyPhen and SIFT, respectively. FASTSNP was used for functional analysis and estimation of risk score. The functional impact on the APOE protein was evaluated by using Swiss PDB viewer and NOMAD-Ref server.Results. Six nsSNPs were found to be least stable by I-Mutant 2.0 with DDG value of >−1.0. Four nsSNPs showed a highly deleterious tolerance index score of 0.00. Nine nsSNPs were found to be probably damaging with position-specific independent counts (PSICs) score of ≥2.0. Seven nsSNPs were found to be highly polymorphic with a risk score of 3-4. The total energies and root-mean-square deviation (RMSD) values were higher for three mutant-type structures compared to the native modeled structure.Conclusion. We concluded that three nsSNPs, namely, rs11542041, rs11542040, and rs11542034, to be potentially functional polymorphic.
机译:介绍。载脂蛋白E(APOE)是阿尔茨海默氏病(AD)的重要危险因素,在30-50%的晚期AD患者中存在。 APOE基因中存在几种单核苷酸多态性(SNP),它们是探索该疾病遗传基础的生物标记。这项研究的目的是鉴定与APOE基因相关的有害nsSNP。从dbSNP中检索了SNP。使用I-Mutant,计算蛋白质稳定性变化。 PolyPhen和SIFT分别预测了潜在功能性非同义(ns)SNP及其对蛋白质的影响。 FASTSNP用于功能分析和风险评分估计。使用Swiss PDB Viewer和NOMAD-Ref服务器评估了对APOE蛋白质的功能影响。 I-Mutant 2.0发现六个nsSNP最不稳定,其DDG值> -1.0。四个nsSNP显示出0.00的高度有害耐受指数。发现九个nsSNP可能具有特定于位置的独立计数(PSIC)得分≥2.0的损害。发现七个nsSNP具有高度多态性,风险评分为3-4。与天然建模结构相比,三种突变型结构的总能量和均方根偏差(RMSD)值更高。我们得出的结论是,三个nsSNP,即rs11542041,rs11542040和rs11542034,具有潜在的功能多态性。

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