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通过体细胞核移植产生的妊娠中期牛胎儿组织中的DNA甲基化模式显示出核重编程中的细微异常。

DNA methylation patterns in tissues from mid-gestation bovine foetuses produced by somatic cell nuclear transfer show subtle abnormalities in nuclear reprogramming.

作者信息

Couldrey Christine, Lee Rita Sf

机构信息

AgResearch, Reproductive Technologies Group, Ruakura Research Centre, East Street, Private Bag 3123, Hamilton, New Zealand.

出版信息

BMC Dev Biol. 2010 Mar 7;10:27. doi: 10.1186/1471-213X-10-27.

Abstract

BACKGROUND

Cloning of cattle by somatic cell nuclear transfer (SCNT) is associated with a high incidence of pregnancy failure characterized by abnormal placental and foetal development. These abnormalities are thought to be due, in part, to incomplete re-setting of the epigenetic state of DNA in the donor somatic cell nucleus to a state that is capable of driving embryonic and foetal development to completion. Here, we tested the hypothesis that DNA methylation patterns were not appropriately established during nuclear reprogramming following SCNT. A panel of imprinted, non-imprinted genes and satellite repeat sequences was examined in tissues collected from viable and failing mid-gestation SCNT foetuses and compared with similar tissues from gestation-matched normal foetuses generated by artificial insemination (AI).

RESULTS

Most of the genomic regions examined in tissues from viable and failing SCNT foetuses had DNA methylation patterns similar to those in comparable tissues from AI controls. However, statistically significant differences were found between SCNT and AI at specific CpG sites in some regions of the genome, particularly those associated with SNRPN and KCNQ1OT1, which tended to be hypomethylated in SCNT tissues. There was a high degree of variation between individuals in methylation levels at almost every CpG site in these two regions, even in AI controls. In other genomic regions, methylation levels at specific CpG sites were tightly controlled with little variation between individuals. Only one site (HAND1) showed a tissue-specific pattern of DNA methylation. Overall, DNA methylation patterns in tissues of failing foetuses were similar to apparently viable SCNT foetuses, although there were individuals showing extreme deviant patterns.

CONCLUSION

These results show that SCNT foetuses that had developed to mid-gestation had largely undergone nuclear reprogramming and that the epigenetic signature at this stage was not a good predictor of whether the foetus would develop to term or not.

摘要

背景

通过体细胞核移植(SCNT)克隆牛与高妊娠失败率相关,其特征为胎盘和胎儿发育异常。这些异常被认为部分是由于供体体细胞核中DNA的表观遗传状态未完全重编程至能够驱动胚胎和胎儿发育至完成的状态。在此,我们检验了以下假设:在SCNT后的核重编程过程中,DNA甲基化模式未得到适当建立。我们检测了一组印记基因、非印记基因和卫星重复序列,这些序列来自妊娠中期存活和失败的SCNT胎儿的组织,并与人工授精(AI)产生的妊娠匹配正常胎儿的类似组织进行比较。

结果

在存活和失败的SCNT胎儿组织中检测的大多数基因组区域,其DNA甲基化模式与AI对照的可比组织中的模式相似。然而,在基因组的某些区域,特别是与SNRPN和KCNQ1OT1相关的区域,SCNT和AI在特定的CpG位点存在统计学上的显著差异,这些区域在SCNT组织中往往发生低甲基化。在这两个区域的几乎每个CpG位点,个体之间的甲基化水平都存在高度差异,即使在AI对照中也是如此。在其他基因组区域,特定CpG位点的甲基化水平受到严格控制,个体之间差异很小。只有一个位点(HAND1)显示出组织特异性的DNA甲基化模式。总体而言,尽管有个体表现出极端异常的模式,但失败胎儿组织中的DNA甲基化模式与明显存活的SCNT胎儿相似。

结论

这些结果表明,发育至妊娠中期的SCNT胎儿在很大程度上已经经历了核重编程,并且这个阶段的表观遗传特征并不能很好地预测胎儿是否会发育至足月。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c661/2848150/be1fba77ae01/1471-213X-10-27-1.jpg

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