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Gene Regulatory Networks Special Feature: Contingent gene regulatory networks and B cell fate specification

机译:基因调控网络的特色:或有基因调控网络和B细胞命运规范

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摘要

The B cell developmental pathway represents a leading system for the analysis of regulatory circuits that orchestrate cell fate specification and commitment. Considerable progress has been achieved within the past decade in the identification and genetic analysis of various regulatory components. These components include the transcription factors PU.1, Ikaros, Bcl11a, E2A, EBF, and Pax-5, as well as the cytokine receptors Flk2 and IL-7R. Experimental evidence of connectivity among the regulatory components is used to assemble sequentially acting and contingent gene regulatory networks. Transient signaling inputs, self-sustaining positive feedback loops, and crossantagonism among alternate cell fate determinants are key features of the proposed networks that instruct the development of B lymphocyte precursors from hematopoietic stem cells.
机译:B细胞的发育途径代表了用于分析调节细胞命运规范和承诺的调节电路的领先系统。在过去的十年中,在鉴定和遗传分析各种调控成分方面已经取得了可观的进步。这些成分包括转录因子PU.1,Ikaros,Bcl11a,E2A,EBF和Pax-5,以及细胞因子受体Flk2和IL-7R。调控元件之间的连通性的实验证据被用于组装顺序起作用的和偶然的基因调控网络。瞬态信号输入,自我维持的正反馈回路以及备用细胞命运决定因素之间的交叉拮抗作用是拟议网络的关键特征,这些网络指示了造血干细胞从B淋巴细胞前体的发育。

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