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首页> 外文期刊>BMC Systems Biology >An organogenesis network-based comparative transcriptome analysis for understanding early human development in vivo and in vitro
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An organogenesis network-based comparative transcriptome analysis for understanding early human development in vivo and in vitro

机译:基于器官发生网络的比较转录组分析,用于了解体内和体外早期人类发育

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Background Integrated networks hold great promise in a variety of contexts. In a recent study, we have combined expression and interaction data to identify a putative network underlying early human organogenesis that contains two modules, the stemness-relevant module (hStemModule) and the differentiation-relevant module (hDiffModule). However, owing to its hypothetical nature, it remains unclear whether this network allows for comparative transcriptome analysis to advance our understanding of early human development, both in vivo and in vitro. Results Based on this integrated network, we here report comparisons with the context-dependent transcriptome data from a variety of sources. By viewing the network and its two modules as gene sets and conducting gene set enrichment analysis, we demonstrate the network's utility as a quantitative monitor of the stem potential versus the differentiation potential. During early human organogenesis, the hStemModule reflects the generality of a gradual loss of the stem potential. The hDiffModule indicates the stage-specific differentiation potential and is therefore not suitable for depicting an extended developmental window. Processing of cultured cells of different types further revealed that the hStemModule is a general indicator that distinguishes different cell types in terms of their stem potential. In contrast, the hDiffModule cannot distinguish between differentiated cells of different types but is able to predict differences in the differentiation potential of pluripotent cells of different origins. We also observed a significant positive correlation between each of these two modules and early embryoid bodies (EBs), which are used as in vitro differentiation models. Despite this, the network-oriented comparisons showed considerable differences between the developing embryos and the EBs that were cultured in vitro over time to try to mimic in vivo processes. Conclusions We strongly recommend the use of these two modules either when pluripotent cell types of different origins are involved or when the comparisons made are constrained to the in vivo embryos during early human organogenesis (and an equivalent in vitro differentiation models). Network-based comparative transcriptome analysis will contribute to an increase in knowledge about human embryogenesis, particularly when only transcriptome data are currently available. These advances will add an extra dimension to network applications.
机译:背景技术集成网络在各种情况下都具有广阔的前景。在最近的一项研究中,我们结合了表达和相互作用数据,以鉴定一个潜在的早期人类器官发生基础网络,该网络包含两个模块:与干性相关的模块(hStemModule)和与分化相关的模块(hDiffModule)。然而,由于其假设性质,目前尚不清楚该网络是否允许进行比较转录组分析以增进我们对体内和体外人类早期发育的了解。结果基于此集成网络,我们在此报告与来自各种来源的上下文相关转录组数据的比较。通过将网络及其两个模块视为基因集并进行基因集富集分析,我们证明了该网络可作为干势与分化势的定量监测器。在人类早期器官形成过程中,hStemModule反映出茎电位逐渐丧失的普遍性。 hDiffModule指示阶段特定的分化潜能,因此不适合描述扩展的发育窗口。对不同类型的培养细胞的加工进一步表明,hStemModule是根据其干潜能区分不同细胞类型的一般指标。相反,hDiffModule无法区分不同类型的分化细胞,但能够预测不同来源的多能细胞分化潜能的差异。我们还观察到这两个模块中的每一个与用作体外分化模型的早期胚状体(EB)之间都存在显着的正相关。尽管如此,面向网络的比较显示,随着时间的流逝,试图模仿体内过程的胚胎和体外培养的EB之间存在很大差异。结论我们强烈建议在涉及不同来源的多能细胞类型时或当在人类早期器官形成过程(以及等效的体外分化模型)中将比较限制在体内胚胎时,建议使用这两个模块。基于网络的比较转录组分析将有助于增加有关人类胚胎发生的知识,特别是在当前仅可获得转录组数据的情况下。这些进步将为网络应用程序增加更多的维度。

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