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A literature-based approach for curating gene signatures in multifaceted diseases

机译:一种基于文献的含有多方面疾病基因特征的方法

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The task of identifying a representative and yet manageable target gene list for assessing the pathogenesis of complicated and multifaceted diseases is challenging. Using Inflammatory Bowel Disease (IBD) as an example, we conceived a bioinformatic approach to identify novel genes associated with the various disease subtypes, in combination with known clinical control genes. From the available literature, we used Acumenta Literature LabTM (LitLab), network analyses, and LitLab Gene Retriever to assemble a gene pool that has a high likelihood of representing immunity-related subtype-specific signatures of IBD. We generated six relevant gene lists and 21 intersections that contain genes with unique literature associations to Crohn’s Disease (n?=?60), Ulcerative Colitis (n?=?17), and unclassified (n?=?45) subtypes of IBD. From this gene pool, we then filtered and constructed, using network analysis, a final list of 142 genes that are the most representative of the disease and its subtypes. In this paper, we present the bioinformatic construction of a gene panel that putatively contains subtype signatures of IBD, a multifactorial disease. These gene signatures will be tested as biomarkers to classify patients with IBD, which has been a clinically challenging task. Such approach to diagnose and monitor complicated disease pathogenesis is a stepping-stone towards personalized care.
机译:鉴定代表性和可管理的目标基因列表的任务,用于评估复杂和多方丝疾病的发病机制是挑战性的。用炎性肠病(IBD)作为一个例子,我们构思了一种生物信息化方法来鉴定与各种疾病亚型相关的新基因,与已知的临床对照基因组合。从可用文献中,我们使用了acumenta文献labtm(Litlab),网络分析和Litlab基因猎犬来组装了具有代表IBD的免疫相关亚型特异性签名的高可能性的基因库。我们生成了六个相关的基因名单和21个交叉点,其含有与克罗恩病的独特文献关联的基因(n?=Δ60),溃疡性结肠炎(n?=Δ17),并且未分类(n?= 45)IBD的亚型。从该基因库中,我们然后通过网络分析过滤和构建并构建了142个基因的最终列表,这是疾病最具代表性及其亚型的基因。在本文中,我们介绍了基因面板的生物信息构建,含有IBD的亚型签名,是多因素疾病。这些基因签名将被视为生物标志物,以对IBD的患者进行分类,这是一个临床挑战的任务。这种诊断和监测复杂疾病发病机制的方法是对个性化护理的踩踏石。

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