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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Virtual Sorting Has a Distinctive Advantage in Identification of Anticorrelated Genes and Further Negative Regulators of Immune Cell Subpopulations
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Virtual Sorting Has a Distinctive Advantage in Identification of Anticorrelated Genes and Further Negative Regulators of Immune Cell Subpopulations

机译:虚拟分类具有独特的优势,在鉴定后环化基因和免疫细胞群的进一步负调节剂

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摘要

Immune cells are highly plastic in both gene expression and cell phenotype. We have established a method of gene expressional plasticity and virtual sorting to evaluate immune cell subpopulations and their characteristic genes in human CD4(+) T cells. In this study, we continued to investigate the informatics mechanism on the effectiveness of virtual sorting. We found that virtual sorting had an overall positive correlation to the Pearson correlation in the identification of positively correlated genes. However, owing to nonlinear biological anticorrelation, virtual sorting showed a distinctive advantage for anticorrelated genes, suggesting an important role in the identification of negative regulators. In addition, based on virtual sorting results, we identified two basic gene sets among highly plastic genes, i.e., highly plastic cell cycle-associated molecules and highly plastic immune and defense response-associated molecules. Genes within each set tended to be positively connected, but genes between two sets were often anticorrelated. Further analysis revealed preferential transcription factor binding motifs existed between highly plastic cell cycle-associated molecules and highly plastic immune and defense response-associated molecules. Our results strongly suggested predetermined regulation, which was called an immune cell internal phenotype, should exist and could be mined by virtual sorting analysis. This provided efficient functional clues to study immune cell phenotypes and their regulation. Moreover, the current substantial virtual sorting results in both CD4(+) T cells and B cells provide a useful resource for big-data-driven experimental studies and knowledge discoveries.
机译:免疫细胞在基因表达和细胞表型中是高度塑料。我们已经建立了一种基因表达可塑性和虚拟分选的方法,以评估人CD4(+)T细胞中的免疫细胞亚群及其特征基因。在这项研究中,我们继续调查关于虚拟分类有效性的信息机制。我们发现,虚拟分类与鉴定正相关基因的Pearson相关性具有总体正相关。然而,由于非线性生物反向吻形成,虚拟分拣对后环化基因显示出独特的优势,这表明在鉴定负调节剂方面的重要作用。另外,基于虚拟分选结果,我们鉴定了高塑料基因中的两个基本基因集,即高度塑料细胞周期相关分子和高度塑性免疫和防御响应相关分子。每个组内的基因倾向于呈正连接,但两组之间的基因往往是非关紧的。进一步的分析显示,在高度塑料细胞周期相关分子和高度塑性免疫和防御响应相关分子之间存在优先转录因子结合基序。我们的结果强烈建议预定调控,称为免疫细胞内部表型,应存在并且可以通过虚拟分选分析开采。这提供了有效的功能线索,以研究免疫细胞表型及其调节。此外,CD4(+)T细胞和B细胞的当前基本的虚拟分类导致CD4(+)T细胞和B细胞提供了对大数据驱动的实验研究和知识发现的有用资源。

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