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Brg1染色质重塑ATP酶通过放大囊胚中期转变时的转录爆发来平衡胚层模式。

Brg1 chromatin remodeling ATPase balances germ layer patterning by amplifying the transcriptional burst at midblastula transition.

作者信息

Wagner Gabriele, Singhal Nishant, Nicetto Dario, Straub Tobias, Kremmer Elisabeth, Rupp Ralph A W

机构信息

Biomedizinisches Zentrum, Molekularbiologie, Ludwig Maximilians-Universität, Großhaderner Strasse 9, Planegg Martinsried, Deutschland.

Bioinformatics Unit, Biomedical Center, Ludwig-Maximilians University, Großhaderner Strasse 9, Planegg Martinsried, Deutschland.

出版信息

PLoS Genet. 2017 May 12;13(5):e1006757. doi: 10.1371/journal.pgen.1006757. eCollection 2017 May.

Abstract

Zygotic gene expression programs control cell differentiation in vertebrate development. In Xenopus, these programs are initiated by local induction of regulatory genes through maternal signaling activities in the wake of zygotic genome activation (ZGA) at the midblastula transition (MBT). These programs lay down the vertebrate body plan through gastrulation and neurulation, and are accompanied by massive changes in chromatin structure, which increasingly constrain cellular plasticity. Here we report on developmental functions for Brahma related gene 1 (Brg1), a key component of embyronic SWI/SNF chromatin remodeling complexes. Carefully controlled, global Brg1 protein depletion in X. tropicalis and X. laevis causes embryonic lethality or developmental arrest from gastrulation on. Transcriptome analysis at late blastula, before development becomes arrested, indicates predominantly a role for Brg1 in transcriptional activation of a limited set of genes involved in pattern specification processes and nervous system development. Mosaic analysis by targeted microinjection defines Brg1 as an essential amplifier of gene expression in dorsal (BCNE/Nieuwkoop Center) and ventral (BMP/Vent) signaling centers. Moreover, Brg1 is required and sufficient for initiating axial patterning in cooperation with maternal Wnt signaling. In search for a common denominator of Brg1 impact on development, we have quantitatively filtered global mRNA fluctuations at MBT. The results indicate that Brg1 is predominantly required for genes with the highest burst of transcriptional activity. Since this group contains many key developmental regulators, we propose Brg1 to be responsible for raising their expression above threshold levels in preparation for embryonic patterning.

摘要

合子基因表达程序控制脊椎动物发育过程中的细胞分化。在非洲爪蟾中,这些程序是在中囊胚转换(MBT)时合子基因组激活(ZGA)之后,通过母体信号活动局部诱导调控基因而启动的。这些程序通过原肠胚形成和神经胚形成奠定脊椎动物的身体蓝图,并伴随着染色质结构的巨大变化,这越来越限制细胞的可塑性。在这里,我们报告了胚胎SWI/SNF染色质重塑复合体的关键成分——与布拉马相关基因1(Brg1)的发育功能。在热带爪蟾和非洲爪蟾中,精心控制的全局Brg1蛋白缺失会导致胚胎致死或从原肠胚形成开始的发育停滞。在发育停滞之前的囊胚后期进行转录组分析表明,Brg1主要在参与模式规范过程和神经系统发育的一组有限基因转录激活中发挥作用。通过靶向显微注射进行的镶嵌分析将Brg1定义为背侧(BCNE/nieuwkoop中心)和腹侧(BMP/vent)信号中心基因表达的必要放大器。此外,Brg1与母体Wnt信号协同启动轴向模式形成是必需的且足够的。为了寻找Brg1对发育影响的共同特征,我们在MBT时定量筛选了全局mRNA波动。结果表明,Brg1主要对转录活性最高的基因是必需的。由于这一组包含许多关键的发育调节因子,我们提出Brg1负责将它们的表达提高到阈值水平以上,为胚胎模式形成做准备。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4d45/5428918/3bb2f7def1c9/pgen.1006757.g001.jpg

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