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Bioinformatics Analysis of Transcriptomic Data Reveals Refined Functional Networks for the Self-Renewal of Mouse Spermatogonial Stem Cells

机译:转录组数据的生物信息学分析揭示了精子功能网络的小鼠精原干细胞的自我更新。

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Spermatogonial stem cells (SSCs) are exquisitely regulated to reach a balance between proliferation and differentiation in the niche of seminiferous epithelium. Several extrinsic factors such as GDNF are reported to switch the transition, activating various intrinsic signaling pathways. Transcriptomics analysis could provide a comprehensive landscape of gene expression and regulation. Here, we reanalyzed a previously published transcriptome of two cell types (standing for self-renewing and differentiating SSCs correspondingly). First, we proposed a new parameter, the expression index, to sort the genes considering both absolute and relative expression levels. Using a dynamic statistical model, we identified a list of 1119 candidate genes for SSC self-renewal with the best enrichment of canonical markers. Finally, based on interaction relations, we further optimized the list and constructed a refined network containing integrated information of interactions, expression alternations, biological functions, and disease associations. Further annotation of the 521 refined genes involved in the network revealed an enrichment of well-studied signaling pathways. We believe that the refined network could help us better understand the regulation of SSCs’ fates, as well as find novel regulators or targets for SSC self-renewal or preservation of male fertility.
机译:精原干细胞(SSCs)受到严格调节,以在生精上皮的利基环境中达到增殖与分化之间的平衡。据报道,诸如GDNF之类的几种外在因素可以转换过渡,激活各种内在的信号传导途径。转录组学分析可以提供基因表达和调控的全面概况。在这里,我们重新分析了先前发布的两种细胞类型的转录组(分别代表自我更新和分化SSC)。首先,我们提出了一个新参数,即表达指数,以考虑绝对和相对表达水平对基因进行分类。使用动态统计模型,我们确定了1119个SSC自我更新候选基因的列表,具有最佳的规范标记丰富性。最后,基于交互关系,我们进一步优化了列表,并构建了一个完善的网络,其中包含交互,表达替代,生物学功能和疾病关联的综合信息。网络中涉及的521个精炼基因的进一步注释揭示了经过充分研究的信号通路。我们认为,完善的网络可以帮助我们更好地了解SSC命运的调控,并找到新颖的SSC自我更新或维持男性生育力的监管者或目标。

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