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拟南芥缺失 BRU1 (维持基因组所必需的)突变体中的异位基因表达和器官发生。

Ectopic gene expression and organogenesis in Arabidopsis mutants missing BRU1 required for genome maintenance.

机构信息

Bioscience and Biotechnology Center, Nagoya University, Chikusa, Nagoya 464-8601, Japan.

出版信息

Genetics. 2011 Sep;189(1):83-95. doi: 10.1534/genetics.111.130062. Epub 2011 Jul 29.

DOI:10.1534/genetics.111.130062
PMID:21705754
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3176131/
Abstract

Chromatin reconstitution after DNA replication and repair is essential for the inheritance of epigenetic information, but mechanisms underlying such a process are still poorly understood. Previously, we proposed that Arabidopsis BRU1 functions to ensure the chromatin reconstitution. Loss-of-function mutants of BRU1 are hypersensitive to genotoxic stresses and cause release of transcriptional gene silencing of heterochromatic genes. In this study, we show that BRU1 also plays roles in gene regulation in euchromatic regions. bru1 mutations caused sporadic ectopic expression of genes, including those that encode master regulators of developmental programs such as stem cell maintenance and embryogenesis. bru1 mutants exhibited adventitious organogenesis, probably due to the misexpression of such developmental regulators. The key regulatory genes misregulated in bru1 alleles were often targets of PcG SET-domain proteins, although the overlap between the bru1-misregulated and PcG SET-domain-regulated genes was limited at a genome-wide level. Surprisingly, a considerable fraction of the genes activated in bru1 were located in several subchromosomal regions ranging from 174 to 944 kb in size. Our results suggest that BRU1 has a function related to the stability of subchromosomal gene regulation in the euchromatic regions, in addition to the maintenance of chromatin states coupled with heritable epigenetic marks.

摘要

染色质在 DNA 复制和修复后进行重组对于表观遗传信息的遗传至关重要,但这一过程的机制仍知之甚少。此前,我们提出拟南芥 BRU1 可确保染色质重组。BRU1 的功能丧失突变体会对遗传毒性压力敏感,并导致异染色质基因转录基因沉默的释放。在这项研究中,我们表明 BRU1 还在常染色质区域的基因调控中发挥作用。bru1 突变导致基因的零星异位表达,包括那些编码发育程序的主要调控因子,如干细胞维持和胚胎发生。bru1 突变体表现出不定器官发生,可能是由于这些发育调控因子的错误表达。在 bru1 等位基因中失调的关键调控基因通常是 PcG SET 结构域蛋白的靶标,尽管在全基因组水平上,bru1 失调和 PcG SET 结构域调控基因之间的重叠有限。令人惊讶的是,在 bru1 中激活的相当一部分基因位于几个亚染色体区域,大小从 174 到 944 kb 不等。我们的结果表明,BRU1 具有与常染色质区域亚染色体基因调控稳定性相关的功能,除了与可遗传表观遗传标记相关的染色质状态维持之外。

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