pyPAGE: A framework for Addressing biases in gene-set enrichment analysis-A case study on Alzheimer's disease.

IF 3.8 2区 生物学 Q1 BIOCHEMICAL RESEARCH METHODS PLoS Computational Biology Pub Date : 2024-09-05 DOI:10.1371/journal.pcbi.1012346
Artemy Bakulin, Noam B Teyssier, Martin Kampmann, Matvei Khoroshkin, Hani Goodarzi
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Abstract

Inferring the driving regulatory programs from comparative analysis of gene expression data is a cornerstone of systems biology. Many computational frameworks were developed to address this problem, including our iPAGE (information-theoretic Pathway Analysis of Gene Expression) toolset that uses information theory to detect non-random patterns of expression associated with given pathways or regulons. Our recent observations, however, indicate that existing approaches are susceptible to the technical biases that are inherent to most real world annotations. To address this, we have extended our information-theoretic framework to account for specific biases and artifacts in biological networks using the concept of conditional information. To showcase pyPAGE, we performed a comprehensive analysis of regulatory perturbations that underlie the molecular etiology of Alzheimer's disease (AD). pyPAGE successfully recapitulated several known AD-associated gene expression programs. We also discovered several additional regulons whose differential activity is significantly associated with AD. We further explored how these regulators relate to pathological processes in AD through cell-type specific analysis of single cell and spatial gene expression datasets. Our findings showcase the utility of pyPAGE as a precise and reliable biomarker discovery in complex diseases such as Alzheimer's disease.

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pyPAGE:解决基因组富集分析中的偏差的框架--关于阿尔茨海默病的案例研究。
从基因表达数据的比较分析中推断驱动调控程序是系统生物学的基石。许多计算框架都是为了解决这个问题而开发的,包括我们的 iPAGE(基因表达的信息理论途径分析)工具集,它利用信息理论检测与给定途径或调控子相关的非随机表达模式。然而,我们最近的观察表明,现有的方法容易受到技术偏差的影响,而技术偏差是大多数现实世界注释的固有特点。为了解决这个问题,我们扩展了信息理论框架,利用条件信息的概念来解释生物网络中的特定偏差和人工痕迹。为了展示 pyPAGE,我们对阿尔茨海默病(AD)分子病因的调控扰动进行了全面分析。我们还发现了另外几个调控子,它们的不同活性与阿兹海默症有显著关联。通过对单细胞和空间基因表达数据集进行细胞类型特异性分析,我们进一步探索了这些调控因子与 AD 病理过程的关系。我们的研究结果展示了 pyPAGE 在阿尔茨海默病等复杂疾病中作为精确可靠的生物标记物发现工具的实用性。
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来源期刊
PLoS Computational Biology
PLoS Computational Biology BIOCHEMICAL RESEARCH METHODS-MATHEMATICAL & COMPUTATIONAL BIOLOGY
CiteScore
7.10
自引率
4.70%
发文量
820
审稿时长
2.5 months
期刊介绍: PLOS Computational Biology features works of exceptional significance that further our understanding of living systems at all scales—from molecules and cells, to patient populations and ecosystems—through the application of computational methods. Readers include life and computational scientists, who can take the important findings presented here to the next level of discovery. Research articles must be declared as belonging to a relevant section. More information about the sections can be found in the submission guidelines. Research articles should model aspects of biological systems, demonstrate both methodological and scientific novelty, and provide profound new biological insights. Generally, reliability and significance of biological discovery through computation should be validated and enriched by experimental studies. Inclusion of experimental validation is not required for publication, but should be referenced where possible. Inclusion of experimental validation of a modest biological discovery through computation does not render a manuscript suitable for PLOS Computational Biology. Research articles specifically designated as Methods papers should describe outstanding methods of exceptional importance that have been shown, or have the promise to provide new biological insights. The method must already be widely adopted, or have the promise of wide adoption by a broad community of users. Enhancements to existing published methods will only be considered if those enhancements bring exceptional new capabilities.
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