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恒河猴-牛种间体细胞核移植胚胎中重编程的转录组。

Reprogrammed transcriptome in rhesus-bovine interspecies somatic cell nuclear transfer embryos.

机构信息

Michigan State University, East Lansing, Michigan, United States of America.

出版信息

PLoS One. 2011;6(7):e22197. doi: 10.1371/journal.pone.0022197. Epub 2011 Jul 25.

Abstract

BACKGROUND

Global activation of the embryonic genome (EGA), one of the most critical steps in early mammalian embryo development, is recognized as the time when interspecies somatic cell nuclear transfer (iSCNT) embryos fail to thrive.

METHODOLOGY/PRINCIPAL FINDINGS: In this study, we analyzed the EGA-related transcriptome of rhesus-bovine iSCNT 8- to 16-cell embryos and dissected the reprogramming process in terms of embryonic gene activation, somatic gene silencing, and maternal RNA degradation. Compared with fibroblast donor cells, two thousand and seven genes were activated in iSCNT embryos, one quarter of them reaching expression levels comparable to those found in in vitro fertilized (IVF) rhesus embryos. This suggested that EGA in iSCNT embryos had partially recapitulated rhesus embryonic development. Eight hundred and sixty somatic genes were not silenced properly and continued to be expressed in iSCNT embryos, which indicated incomplete nuclear reprogramming. We compared maternal RNA degradation in bovine oocytes between bovine-bovine SCNT and iSCNT embryos. While maternal RNA degradation occurred in both SCNT and iSCNT embryos, we saw more limited overall degradation of maternal RNA in iSCNT embryos than in SCNT embryos. Several important maternal RNAs, like GPF9, were not properly processed in SCNT embryos.

CONCLUSIONS/SIGNIFICANCE: Our data suggested that iSCNT embryos are capable of triggering EGA, while a portion of somatic cell-associated genes maintain their expression. Maternal RNA degradation seems to be impaired in iSCNT embryos. Further understanding of the biological roles of these genes, networks, and pathways revealed by iSCNT may expand our knowledge about cell reprogramming, pluripotency, and differentiation.

摘要

背景

胚胎基因组的全球激活(EGA)是早期哺乳动物胚胎发育过程中最关键的步骤之一,被认为是种间体细胞核移植(iSCNT)胚胎无法存活的时间点。

方法/主要发现:在这项研究中,我们分析了猕猴-牛 iSCNT 8-16 细胞胚胎的 EGA 相关转录组,并根据胚胎基因激活、体细胞基因沉默和母源 RNA 降解来剖析重编程过程。与成纤维细胞供体细胞相比,2007 个基因在 iSCNT 胚胎中被激活,其中四分之一的基因达到了与体外受精(IVF)猕猴胚胎相当的表达水平。这表明 iSCNT 胚胎的 EGA 部分再现了猕猴胚胎的发育。860 个体细胞基因没有被正确沉默,继续在 iSCNT 胚胎中表达,这表明核重编程不完全。我们比较了牛卵母细胞中牛-牛 SCNT 和 iSCNT 胚胎之间的母源 RNA 降解。虽然母源 RNA 降解发生在 SCNT 和 iSCNT 胚胎中,但我们发现 iSCNT 胚胎中母源 RNA 的总体降解更为有限。一些重要的母源 RNA,如 GPF9,在 SCNT 胚胎中没有被正确加工。

结论/意义:我们的数据表明,iSCNT 胚胎能够触发 EGA,而一部分体细胞相关基因保持表达。母源 RNA 降解似乎在 iSCNT 胚胎中受到损害。进一步了解 iSCNT 揭示的这些基因、网络和途径的生物学作用可能会扩展我们对细胞重编程、多能性和分化的认识。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/274a/3143123/ca90ad8e11b1/pone.0022197.g001.jpg

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