Broad Institute of MIT and Harvard, 7 Cambridge Center, Cambridge, Massachusetts 02142, USA.
Nature. 2013 Apr 25;496(7446):461-8. doi: 10.1038/nature11981. Epub 2013 Mar 6.
Despite their importance, the molecular circuits that control the differentiation of naive T cells remain largely unknown. Recent studies that reconstructed regulatory networks in mammalian cells have focused on short-term responses and relied on perturbation-based approaches that cannot be readily applied to primary T cells. Here we combine transcriptional profiling at high temporal resolution, novel computational algorithms, and innovative nanowire-based perturbation tools to systematically derive and experimentally validate a model of the dynamic regulatory network that controls the differentiation of mouse TH17 cells, a proinflammatory T-cell subset that has been implicated in the pathogenesis of multiple autoimmune diseases. The TH17 transcriptional network consists of two self-reinforcing, but mutually antagonistic, modules, with 12 novel regulators, the coupled action of which may be essential for maintaining the balance between TH17 and other CD4(+) T-cell subsets. Our study identifies and validates 39 regulatory factors, embeds them within a comprehensive temporal network and reveals its organizational principles; it also highlights novel drug targets for controlling TH17 cell differentiation.
尽管它们很重要,但控制初始 T 细胞分化的分子回路在很大程度上仍是未知的。最近的研究重建了哺乳动物细胞中的调控网络,这些研究主要集中在短期反应上,并且依赖于基于扰动的方法,这些方法不能轻易应用于原代 T 细胞。在这里,我们结合高时间分辨率的转录谱分析、新颖的计算算法和创新的基于纳米线的扰动工具,系统地推导和实验验证了一个控制小鼠 TH17 细胞分化的动态调控网络模型,TH17 细胞是一种促炎性 T 细胞亚群,与多种自身免疫性疾病的发病机制有关。TH17 转录网络由两个自我强化但相互拮抗的模块组成,包含 12 个新的调节剂,它们的耦合作用对于维持 TH17 和其他 CD4+T 细胞亚群之间的平衡可能是必不可少的。我们的研究鉴定和验证了 39 个调节因子,将它们嵌入一个全面的时间网络中,并揭示了其组织原则;它还突出了控制 TH17 细胞分化的新药物靶点。
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