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通过凝聚素 II 复合物进行染色质凝聚是外周 T 细胞静止所必需的。

Chromatin condensation via the condensin II complex is required for peripheral T-cell quiescence.

机构信息

Department of Biochemistry, St Jude Children's Research Hospital, Memphis, TN, USA.

出版信息

EMBO J. 2011 Jan 19;30(2):263-76. doi: 10.1038/emboj.2010.314. Epub 2010 Dec 17.

Abstract

Naive T cells encountering their cognate antigen become activated and acquire the ability to proliferate in response to cytokines. Stat5 is an essential component in this response. We demonstrate that Stat5 cannot access DNA in naive T cells and acquires this ability only after T-cell receptor (TCR) engagement. The transition is not associated with changes in DNA methylation or global histone modification but rather chromatin decondensation. Condensation occurs during thymocyte development and proper condensation is dependent on kleisin-β of the condensin II complex. Our findings suggest that this unique chromatin condensation, which can affect interpretations of chromatin accessibility assays, is required for proper T-cell development and maintenance of the quiescent state. This mechanism ensures that cytokine driven proliferation can only occur in the context of TCR stimulation.

摘要

幼稚 T 细胞遇到其同源抗原后被激活,并获得对细胞因子增殖的能力。Stat5 是该反应的一个重要组成部分。我们证明,Stat5 无法在幼稚 T 细胞中访问 DNA,并且仅在 T 细胞受体(TCR)结合后才获得此能力。这种转变与 DNA 甲基化或组蛋白整体修饰的变化无关,而是与染色质解凝聚有关。凝聚发生在胸腺细胞发育过程中,适当的凝聚取决于凝聚素 II 复合物的 kleisin-β。我们的研究结果表明,这种独特的染色质凝聚,可能会影响对染色质可及性测定的解释,是适当的 T 细胞发育和维持静止状态所必需的。该机制确保细胞因子驱动的增殖只能在 TCR 刺激的情况下发生。

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