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首页> 外文期刊>Russian Journal of Developmental Biology >Effect of 5-azadeoxycytidine and retinoic acid on expression of genomic imprinting in parthenogenetic mouse embryos
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Effect of 5-azadeoxycytidine and retinoic acid on expression of genomic imprinting in parthenogenetic mouse embryos

机译:5-氮杂脱氧胞苷和视黄酸对孤雌小鼠胚胎基因组印迹表达的影响

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摘要

The action of two types of substances has been studied: 5-azadeoxycytidine and retinoic acid, which have a demethylation effect on DNA in the development process of diploid parthenogenetic mouse embryos. The effect of 5-azadeoxycytidine on hybrid mice (CBA x C57BL/6)F1 in vitro for 6 h, in the presence of single cell parthenogenetic embryos during the S-phase of the cell cycle has been studied. After developing to the blastocyst stage in vitro, parthenogenetic embryos were transplanted into the uterus of false pregnant females. It has been determined that a concentration of 0.1 mu M 5-azadeoxycytidine activates embryonic development in the preimplantation period until the blastocyst stage (69% in experiment; 61% in the control) and during postimplantation, it increases the number of available space in the uterus for implantation (76% in experiment; 63% in the control).The effect of retinoic acid on parthenogenetic embryos from inbred C57BL/6 or CBA mice lines was studied by adding it to single cell embryos in a medium in vitro for 96 h. Treating parthenogenetic embryos C57BL/6 with retinoic acid concentrations 0.1 mu M or 0.5 mu M significantly increased the number of spaces for embryo implantation, 76% and 78% respectively, as against 57% for untreated embryos. Addition of similar doses of retinoic acid to the nutrient medium containing CBA parthenogenetic mouse embryos does not improve implantation (as with embryos C57BL/6), and a concentration of 2.0 mu M is toxic to the embryos. During the period of postimplantation, parthenogenetic embryos of mouse lines C57BL/6 treated with retinoic acid just as the controls, did not develop to the somite stage. Mouse lines CBA had 45% of their embryos which were used as controls, developing to the advanced somite stages. However, the number of embryos treated with retinoic acid does not increase. Thus the treatment of two parthenogenetic embryos from inbred mice lines and their hybrids with compounds which demethylate DNA (5-azadeoxycytidine and retinoic acid) creates an opportunity for partial modulation of genomic imprinting and an increase in the survival rate of such embryos.
机译:已经研究了两种物质的作用:5-氮杂脱氧胞苷和视黄酸,它们在二倍体孤雌生殖小鼠胚胎的发育过程中对DNA具有去甲基作用。研究了5-氮杂脱氧胞苷在单细胞孤雌生殖胚胎在细胞周期S期存在的情况下,对杂种小鼠(CBA x C57BL / 6)F1的体外作用6 h。在体外发育到胚泡期后,将孤雌生殖胚胎移植到假孕妇的子宫中。已确定浓度为0.1μM的5-氮杂脱氧胞苷在植入前直至胚泡阶段(实验中为69%;对照中为61%)和在植入后期间激活了胚胎发育,从而增加了胚胎中的可用空间数量。通过在体外培养基中将视黄酸添加到离体C57BL / 6或CBA小鼠品系的孤雌生殖胚胎中体外培养96小时,研究了视黄酸对单性生殖胚胎的影响。用0.1μM或0.5μM的视黄酸浓度处理孤雌生殖胚胎C57BL / 6,显着增加了胚胎植入空间的数量,分别为76%和78%,而未处理的胚胎为57%。向含有CBA单性生殖小鼠胚胎的营养培养基中添加相似剂量的视黄酸并不能改善植入效果(与C57BL / 6胚胎一样),并且2.0μM的浓度对胚胎有毒。在植入后的期间,以视黄酸作为对照处理的小鼠品系C57BL / 6的孤雌生殖胚胎没有发育到体节期。小鼠品系CBA的胚胎中有45%被用作对照,发展到晚期松脱阶段。但是,用视黄酸处理的胚胎数量并未增加。因此,用脱甲基化DNA的化合物(5-氮杂脱氧胞苷和视黄酸)处理近交小鼠品系及其杂种的两个孤雌生殖胚胎,为部分调节基因组印迹和增加此类胚胎的存活率提供了机会。

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