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Age-associated chromatin relaxation is enhanced in Huntingtons disease mice

机译:亨廷顿病小鼠中与年龄相关的染色质松弛增强

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摘要

Expansion of polyglutamine stretch in the huntingtin (HTT) protein is a major cause of Huntington's disease (HD). The polyglutamine part in HTT interacts with various proteins implicated in epigenetic regulation of genes, suggesting that mutant HTT may disturb the integrity of the epigenetic system. Here, we used a PCRseq-based method to examine expression profile of 395 exonic segments from 260 “epi-driver” genes in splenic T lymphocytes from aged HD mice. We identified 67 exonic segments differentially expressed between young and aged HD mice, most of them upregulated in the aged. Polycomb-repressive complex (PRC)-regulated genes (PRGs) were markedly upregulated in aged HD mice, consistent with downregulation of PRC genes. Epi-driver gene categories of lysine-methylation, lysine-demethylation, arginine-methylation, and PRG showed differential age-associated changes between HD and control. Analyzing the pattern of change in epi-driver gene expressions hinted at an enhanced shift in HD chromatin to a more accessible state with age, which was experimentally demonstrated by DNase-I-hypersensitivity sequencing showing increased chromatin accessibility in HD cells compared to control. We suggest the global change can potentially relieve chromatin-induced repression of many genes, and the unintended expressions of some detrimental proteins could alter T cell function to a greater degree in aged HD mice.
机译:亨廷顿蛋白(HTT)蛋白中聚谷氨酰胺的扩展是亨廷顿舞蹈病(HD)的主要原因。 HTT中的聚谷氨酰胺部分与涉及基因的表观遗传调控的各种蛋白质相互作用,这表明突变型HTT可能会干扰表观遗传系统的完整性。在这里,我们使用了一种基于PCRseq的方法来检查来自年龄较大的HD小鼠的脾T淋巴细胞中260个“ epi-driver”基因中395个外显子片段的表达谱。我们确定了67个外显子片段在年轻和老年HD小鼠之间差异表达,其中大多数在老年人中表达上调。在老年HD小鼠中,多梳抑制复合物(PRC)调控的基因(PRGs)明显上调,与PRC基因的下调一致。赖氨酸甲基化,赖氨酸脱甲基化,精氨酸甲基化和PRG的Epi-driver基因类别显示HD和对照之间存在不同的年龄相关变化。分析Epi-Driver基因表达的变化模式表明,随着年龄的增长,HD染色质向更易接近的状态转移的增强,这由DNase-I超敏测序证实,与对照组相比,HD细胞的染色质可访问性增加。我们认为,这种全局变化可以潜在地缓解染色质诱导的许多基因的抑制,而某些有害蛋白质的意外表达可能会在老年HD小鼠中更大程度地改变T细胞的功能。

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