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Germline-specific epigenetic reprogramming of primary epimutations in mice produced by assisted reproductive technology.

机译:通过辅助生殖技术产生的小鼠原发性表皮生殖细胞特异性表观遗传重编程。

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摘要

Assistive reproductive technologies (ART) including intra-cytoplasmic sperm injection (ICSI) are now commonly used in human and other animals. However, epigenetic defects have been in individuals produced by ART. Interestingly, in animal studies, epigenetic defects observed in individuals produced by ART are typically not transmitted to progeny produced by natural reproduction. This suggests that these defects are corrected by germline-specific epigenetic reprogramming, but this has not previously been directly demonstrated experimentally. To investigate this further, we examined three imprinted genes, H19 , Snrpn and Peg3 to assess the occurrence of epimutations in mice produce by intracytoplasmic sperm injection (ICSI—a form of ART), and the subsequent correction of these epimutations in the germ line. We examined allele-specific DNA methylation profiles in differentially methylated regions (DMRs) of these genes, as well as allele-specific expression of these genes in somatic cells and germ cells. We found that - primary epimutations and correlated abnormal expression were present in many of the samples obtained from mice generated by ICSI, but not in any of the naturally conceived mice. We further observed that following natural mating of the ICSI mice, these epimutations were not transmitted to offspring. Subsequent analysis of germ cells from the ICSI mice revealed that the epimutations were corrected by germline-specific reprogramming. Additional analyses of epigenetic profiles of imprinted genes in ICSI mice at 6 days postpartum (dpp), as well as in mice produced from oocytes that had undergone endocrine stimulation followed by natural insemination implicate endocrine stimulation (superovulation) as one causative agent leading to primary epimutations in ART mice.
机译:辅助生殖技术(ART)包括胞浆内精子注射(ICSI)现在普遍用于人类和其他动物。然而,表观遗传缺陷存在于ART产生的个体中。有趣的是,在动物研究中,在ART产生的个体中观察到的表观遗传缺陷通常不会传播至自然繁殖产生的后代。这表明这些缺陷已通过种系特异性表观遗传重编程得到纠正,但是以前尚未通过实验直接证明。为了进一步研究这一问题,我们检查了三个印迹基因H19,Snrpn和Peg3,以评估通过胞浆内精子注射(ICSI-ART的一种形式)产生的小鼠表位突变的发生,以及随后对种系中这些表位突变的纠正。我们检查了这些基因的差异甲基化区域(DMR)中的等位基因特异性DNA甲基化谱,以及这些基因在体细胞和生殖细胞中的等位基因特异性表达。我们发现-从ICSI生成的小鼠中获得的许多样品中都存在原发性表位突变和相关的异常表达,但在任何自然受孕的小鼠中都没有。我们进一步观察到,ICSI小鼠自然交配后,这些表位变异并未传播给后代。随后对来自ICSI小鼠的生殖细胞的分析表明,通过种系特异性重编程可以纠正表观突变。对产后6天(dpp)的ICSI小鼠以及经过内分泌刺激后自然授精的卵母细胞产生的小鼠中印迹基因的表观遗传学特征的其他分析表明,内分泌刺激(超排卵)是导致主要表位突变的一种病因在ART小鼠中。

著录项

  • 作者

    Ingale, Puraskar Narendra.;

  • 作者单位

    The University of Texas at San Antonio.;

  • 授予单位 The University of Texas at San Antonio.;
  • 学科 Biology Molecular.;Biology Genetics.
  • 学位 M.S.
  • 年度 2011
  • 页码 51 p.
  • 总页数 51
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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