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An incoherent regulatory network architecture that orchestrates B cell diversification in response to antigen signaling

机译:不协调的调节网络体系结构可响应抗原信号传导而协调B细胞的多样化

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摘要

The B-lymphocyte lineage is a leading system for analyzing gene regulatory networks (GRNs) that orchestrate distinct cell fate transitions. Upon antigen recognition, B cells can diversify their immunoglobulin (Ig) repertoire via somatic hypermutation (SHM) and/or class switch DNA recombination (CSR) before differentiating into antibody-secreting plasma cells. We construct a mathematical model for a GRN underlying this developmental dynamic. The intensity of signaling through the Ig receptor is shown to control the bimodal expression of a pivotal transcription factor, IRF-4, which dictates B cell fate outcomes. Computational modeling coupled with experimental analysis supports a model of ‘kinetic control', in which B cell developmental trajectories pass through an obligate transient state of variable duration that promotes diversification of the antibody repertoire by SHM/CSR in direct response to antigens. More generally, this network motif could be used to translate a morphogen gradient into developmental inductive events of varying time, thereby enabling the specification of distinct cell fates.
机译:B淋巴细胞谱系是分析基因调控网络(GRN)的领先系统,这些基因调控网络可协调不同的细胞命运转换。抗原识别后,B细胞可以在分化为分泌抗体的浆细胞之前,通过体细胞超突变(SHM)和/或类别开关DNA重组(CSR)使免疫球蛋白(Ig)种类多样化。我们为这一发展动态基础的GRN构建数学模型。显示通过Ig受体的信号传导强度可控制关键转录因子IRF-4的双峰表达,这决定了B细胞的命运。计算模型与实验分析相结合,为“动力学控制”模型提供了支持,其中B细胞的发展轨迹经过了持续时间可变的专性瞬态,从而促进了SHM / CSR对抗原的直接反应,从而使抗体库多样化。更一般地,该网络基序可用于将形态发生子梯度转化为不同时间的发育诱导事件,从而能够确定不同的细胞命运。

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