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Genome-Wide Analysis of Abnormal H3K9 Acetylation in Cloned Mice

机译:克隆小鼠H3K9乙酰化异常的全基因组分析

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摘要

Somatic nuclear transfer is a cloning technique that shows great promise in the application to regenerative medicine. Although cloned animals are genetically identical to their donor counterparts, abnormalities in phenotype and gene expression are frequently observed. One hypothesis is that the cause of these abnormalities is due to epigenetic aberration. In this report, we focused our analysis on the acetylation of histone H3 at lysine9 (H3K9Ac). Through the use of whole genome tiling arrays and quantitative PCR, we examined this epigenetic event and directly compared and assessed the differences between a cloned mouse (C1) and its parental nuclear donor (D1) counterpart. We identified 4720 regions of chromosomal DNA that showed notable differences in H3K9Ac and report here many genes identified in these hyper- and hypo-acetylated regions. Analysis of a second clone (C2) and its parental donor counterpart (D2) for H3K9Ac showed a high degree of similarity to the C1/D1 pair. This conservation of aberrant acetylation is suggestive of a reproducible epigenetic phenomenon that may lead to the frequent abnormalities observed in cloned mice, such as obesity. Furthermore, we demonstrated Crp which was identified as a hyper-acetylated gene in this study is related to the body mass, suggesting that Crp is a possible candidate of a cause for the abnormal obesity in cloned mice. In this, one of the first reports describing genome-wide epigenetic abberation between parental and nuclear transfer-cloned mammals, we propose that aberrant acetylation of histones (H3K9Ac) flanking promoter regions highly correlates with gene-expression and may itself be an epigenetic change that accounts for variable expression patterns observed in cloned animals.
机译:体细胞核移植是一种克隆技术,在再生医学中显示出巨大的希望。尽管克隆的动物与供体的动物在基因上相同,但经常观察到表型和基因表达异常。一种假设是这些异常的原因是由于表观遗传畸变。在本报告中,我们将分析重点放在组氨酸H3在赖氨酸9(H3K9Ac)的乙酰化上。通过使用全基因组切片阵列和定量PCR,我们检查了这种表观遗传事件,并直接比较和评估了克隆的小鼠(C1)和其亲代核供体(D1)之间的差异。我们鉴定了在H3K9Ac中显示出显着差异的染色体DNA的4720个区域,并在此报告了在这些高乙酰和低乙酰化区域中鉴定出的许多基因。对H3K9Ac的第二个克隆(C2)及其亲本供体对应物(D2)的分析显示,与C1 / D1对高度相似。异常乙酰化的这种保守性暗示可再现的表观遗传现象,其可能导致在克隆的小鼠中观察到频繁的异常,例如肥胖。此外,我们证明了在该研究中被鉴定为高乙酰化基因的Crp与体重有关,这表明Crp是克隆小鼠中异常肥胖病因的可能候选者。在此中,描述亲本和核转移克隆的哺乳动物之间全基因组表观遗传变异的第一份报告之一,我们提出组蛋白(H3K9Ac)侧翼启动子区域的异常乙酰化与基因表达高度相关,并且本身可能是表观遗传变化,解释了在克隆动物中观察到的可变表达模式。

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