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染色质引发元件在不激活转录的情况下在T细胞中建立免疫记忆:T细胞记忆由DNA元件维持,这些元件稳定地引发可诱导基因而不激活稳态转录。

Chromatin priming elements establish immunological memory in T cells without activating transcription: T cell memory is maintained by DNA elements which stably prime inducible genes without activating steady state transcription.

作者信息

Bevington Sarah L, Cauchy Pierre, Cockerill Peter N

机构信息

Institute of Cancer and Genomic Sciences, Institute of Biomedical Research, University of Birmingham, Birmingham, West Midlands, UK.

出版信息

Bioessays. 2017 Feb;39(2). doi: 10.1002/bies.201600184. Epub 2016 Dec 27.

Abstract

We have identified a simple epigenetic mechanism underlying the establishment and maintenance of immunological memory in T cells. By studying the transcriptional regulation of inducible genes we found that a single cycle of activation of inducible factors is sufficient to initiate stable binding of pre-existing transcription factors to thousands of newly activated distal regulatory elements within inducible genes. These events lead to the creation of islands of active chromatin encompassing nearby enhancers, thereby supporting the accelerated activation of inducible genes, without changing steady state levels of transcription in memory T cells. These studies also highlighted the need for more sophisticated definitions of gene regulatory elements. The chromatin priming elements defined here are distinct from classical enhancers because they function by maintaining chromatin accessibility rather than directly activating transcription. We propose that these priming elements are members of a wider class of genomic elements that support correct developmentally regulated gene expression.

摘要

我们已经确定了一种简单的表观遗传机制,该机制是T细胞免疫记忆建立和维持的基础。通过研究诱导基因的转录调控,我们发现诱导因子的单个激活周期足以启动预先存在的转录因子与诱导基因内数千个新激活的远端调控元件的稳定结合。这些事件导致包含附近增强子的活性染色质岛的形成,从而支持诱导基因的加速激活,而不改变记忆T细胞中的转录稳态水平。这些研究还强调了对基因调控元件进行更精确定义的必要性。这里定义的染色质启动元件与经典增强子不同,因为它们通过维持染色质可及性而非直接激活转录来发挥作用。我们提出这些启动元件是支持正确的发育调控基因表达的更广泛基因组元件类别的成员。

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