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应用证据权重法评估暴露-疾病范式中分子格局的相关性。

Applying a Weight-of-Evidence Approach to Evaluate Relevance of Molecular Landscapes in the Exposure-Disease Paradigm.

作者信息

Gross Sherilyn A, Fedak Kristen M

机构信息

Cardno ChemRisk, 4840 Pearl East Circle 300 W., Boulder, CO 80304, USA.

Department of Environmental & Radiological Health Sciences, Colorado State University, Fort Collins, CO 80523, USA.

出版信息

Biomed Res Int. 2015;2015:515798. doi: 10.1155/2015/515798. Epub 2015 Aug 3.

Abstract

Information on polymorphisms, mutations, and epigenetic events has become increasingly important in our understanding of molecular mechanisms associated with exposures-disease outcomes. Molecular landscapes can be developed to illustrate the molecular characteristics for environmental carcinogens as well as associated disease outcomes, although comparison of these molecular landscapes can often be difficult to navigate. We developed a method to organize these molecular data that uses a weight-of-evidence approach to rank overlapping molecular events by relative importance for susceptibility to an exposure-disease paradigm. To illustrate the usefulness of this approach, we discuss the example of benzene as an environmental carcinogen and myelodysplastic syndrome (MDS) as a causative disease endpoint. Using this weight-of-evidence method, we found overlapping polymorphisms in the genes for the metabolic enzymes GST and NQO1, both of which may infer risk of benzene-induced MDS. Polymorphisms in the tumor suppressor gene, TP53, and the inflammatory cytokine gene, TNF-α, were also noted, albeit inferring opposing outcomes. The alleles identified in the DNA repair gene RAD51 indicated an increased risk for MDS in MDS patients and low blood cell counts in benzene-exposed workers. We propose the weight-of-evidence approach as a tool to assist in organizing the sea of emerging molecular data in exposure-disease paradigms.

摘要

关于多态性、突变和表观遗传事件的信息,在我们理解与暴露-疾病结局相关的分子机制方面变得越来越重要。可以构建分子图谱来说明环境致癌物的分子特征以及相关的疾病结局,尽管这些分子图谱的比较往往很难进行。我们开发了一种方法来整理这些分子数据,该方法采用证据权重法,根据对暴露-疾病模式易感性的相对重要性对重叠的分子事件进行排序。为了说明这种方法的实用性,我们讨论了以苯作为环境致癌物、骨髓增生异常综合征(MDS)作为致病疾病终点的例子。使用这种证据权重法,我们在代谢酶GST和NQO1的基因中发现了重叠的多态性,这两者都可能提示苯诱导的MDS的风险。肿瘤抑制基因TP53和炎性细胞因子基因TNF-α中的多态性也被注意到,尽管提示了相反的结果。在DNA修复基因RAD51中鉴定出的等位基因表明,MDS患者患MDS的风险增加,且苯暴露工人的血细胞计数较低。我们提出将证据权重法作为一种工具,以协助整理暴露-疾病模式中大量新出现的分子数据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c716/4538402/d72cd38bab94/BMRI2015-515798.001.jpg

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