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Bioinformatics Identification of Modules of Transcription Factor Binding Sites in Alzheimer's Disease-Related Genes by In Silico Promoter Analysis and Microarrays

机译:通过计算机启动子分析和微阵列鉴定阿尔茨海默氏病相关基因中转录因子结合位点模块的生物信息学。

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摘要

The molecular mechanisms and genetic risk factors underlying Alzheimer's disease (AD) pathogenesis are only partly understood. To identify new factors, which may contribute to AD, different approaches are taken including proteomics, genetics, and functional genomics. Here, we used a bioinformatics approach and found that distinct AD-related genes share modules of transcription factor binding sites, suggesting a transcriptional coregulation. To detect additional coregulated genes, which may potentially contribute to AD, we established a new bioinformatics workflow with known multivariate methods like support vector machines, biclustering, and predicted transcription factor binding site modules by using in silico analysis and over 400 expression arrays from human and mouse. Two significant modules are composed of three transcription factor families: CTCF, SP1F, and EGRF/ZBPF, which are conserved between human and mouse APP promoter sequences. The specific combination of in silico promoter and multivariate analysis can identify regulation mechanisms of genes involved in multifactorial diseases.
机译:阿尔茨海默氏病(AD)发病机理的分子机制和遗传危险因素仅被部分了解。为了确定可能导致AD的新因素,采用了不同的方法,包括蛋白质组学,遗传学和功能基因组学。在这里,我们使用了生物信息学方法,发现不同的AD相关基因共享转录因子结合位点的模块,提示转录共调控。为了检测可能潜在地导致AD的其他共调节基因,我们使用计算机模拟和超过400种来自人类和人类的表达阵列,通过已知的多变量方法(例如支持载体机,双聚簇和预测的转录因子结合位点模块)建立了新的生物信息学工作流程。老鼠。两个重要的模块由三个转录因子家族组成:CTCF,SP1F和EGRF / ZBPF,在人和小鼠APP启动子序列之间保守。计算机启动子和多变量分析的特定组合可以确定涉及多因素疾病的基因的调控机制。

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