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胎儿和成年前T细胞发育过程中调控基因表达状态的进展。

Progression of regulatory gene expression states in fetal and adult pro-T-cell development.

作者信息

David-Fung Elizabeth-Sharon, Yui Mary A, Morales Marissa, Wang Hua, Taghon Tom, Diamond Rochelle A, Rothenberg Ellen V

机构信息

Division of Biology, California Institute of Technology, Pasadena, CA 91125, USA.

出版信息

Immunol Rev. 2006 Feb;209:212-36. doi: 10.1111/j.0105-2896.2006.00355.x.

DOI:10.1111/j.0105-2896.2006.00355.x
PMID:16448545
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4157939/
Abstract

Precursors entering the T-cell developmental pathway traverse a progression of states characterized by distinctive patterns of gene expression. Of particular interest are regulatory genes, which ultimately control the dwell time of cells in each state and establish the mechanisms that propel them forward to subsequent states. Under particular genetic and developmental circumstances, the transitions between these states occur with different timing, and environmental feedbacks may shift the steady-state accumulations of cells in each state. The fetal transit through pro-T-cell stages is faster than in the adult and subject to somewhat different genetic requirements. To explore causes of such variation, this review presents previously unpublished data on differentiation gene activation in pro-T cells of pre-T-cell receptor-deficient mutant mice and a quantitative comparison of the profiles of transcription factor gene expression in pro-T-cell subsets of fetal and adult wildtype mice. Against a background of consistent gene expression, several regulatory genes show marked differences between fetal and adult expression profiles, including those encoding two basic helix-loop-helix antagonist Id factors, the Ets family factor SpiB and the Notch target gene Deltex1. The results also reveal global differences in regulatory alterations triggered by the first T-cell receptor-dependent selection events in fetal and adult thymopoiesis.

摘要

进入T细胞发育途径的前体细胞会经历一系列以独特基因表达模式为特征的状态。特别值得关注的是调控基因,它们最终控制细胞在每个状态下的停留时间,并建立推动细胞进入后续状态的机制。在特定的遗传和发育环境下,这些状态之间的转变发生时间不同,环境反馈可能会改变每个状态下细胞的稳态积累。胎儿通过前T细胞阶段的过程比成人更快,并且受到一些不同的遗传要求的影响。为了探究这种差异的原因,本综述展示了关于前T细胞受体缺陷突变小鼠前T细胞中分化基因激活的未发表数据,以及胎儿和成年野生型小鼠前T细胞亚群中转录因子基因表达谱的定量比较。在一致的基因表达背景下,几个调控基因在胎儿和成人表达谱之间表现出明显差异,包括编码两种基本螺旋-环-螺旋拮抗剂Id因子、Ets家族因子SpiB和Notch靶基因Deltex1的基因。结果还揭示了胎儿和成人胸腺生成中首次T细胞受体依赖性选择事件引发的调控改变的全局差异。

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