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A genome-wide regulatory network identifies key transcription factors for memory CD8+ T-cell development

机译:全基因组调控网络识别记忆CD8 + T细胞发育的关键转录因子

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摘要

Memory CD8[superscript +] T-cell development is defined by the expression of a specific set of memory signature genes. Despite recent progress, many components of the transcriptional control of memory CD8[superscript +] T-cell development are still unknown. To identify transcription factors and their interactions in memory CD8[superscript +] T-cell development, we construct a genome-wide regulatory network and apply it to identify key transcription factors that regulate memory signature genes. Most of the known transcription factors having a role in memory CD8[superscript +] T-cell development are rediscovered and about a dozen new ones are also identified. Sox4, Bhlhe40, Bach2 and Runx2 are experimentally verified, and Bach2 is further shown to promote both development and recall proliferation of memory CD8[superscript +] T cells through Prdm1 and Id3. Gene perturbation study identifies the interactions between the transcription factors, with Sox4 positioned as a hub. The identified transcription factors and insights into their interactions should facilitate further dissection of molecular mechanisms underlying memory CD8[superscript +] T-cell development.
机译:记忆CD8 + T细胞的发育由一组特定的记忆特征基因的表达来定义。尽管有最近的进展,但是记忆CD8 + T细胞发育的转录控制的许多组件仍是未知的。为了鉴定转录因子及其在记忆CD8 + T细胞发育中的相互作用,我们构建了一个全基因组调控网络,并将其应用于鉴定调控记忆信号基因的关键转录因子。重新发现了大多数在记忆CD8 + T细胞发育中起作用的已知转录因子,还鉴定了大约12个新的转录因子。通过实验验证了Sox4,Bhlhe40,Bach2和Runx2,并且进一步证明了Bach2可以通过Prdm1和Id3促进记忆CD8 ^ + T细胞的发育并促进其增殖。基因扰动研究确定了转录因子之间的相互作用,其中Sox4被定位为枢纽。鉴定出的转录因子及其相互作用的见解应有助于进一步剖析记忆CD8 [上标+] T细胞发育的分子机制。

著录项

  • 作者

    Hu Guangan; Chen Jianzhu;

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  • 年度 2013
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  • 原文格式 PDF
  • 正文语种 en_US
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