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首页> 外文期刊>Cellular reprogramming >Treatment of Nuclear-Donor Cells or Cloned Zygotes with Chromatin-Modifying Agents Increases Histone Acetylation But Does Not Improve Full-Term Development of Cloned Cattle
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Treatment of Nuclear-Donor Cells or Cloned Zygotes with Chromatin-Modifying Agents Increases Histone Acetylation But Does Not Improve Full-Term Development of Cloned Cattle

机译:用染色质修饰剂处理核供体细胞或克隆合子增加组蛋白乙酰化,但不能改善克隆牛的长期发育

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Although somatic cell nuclear transfer (SCNT) is a promising tool, its potential use is hampered by the high mortality rates during the development to term of cloned offspring. Abnormal epigenetic reprogramming of donor nuclei after SCNT is thought to be the main cause of this low efficiency. We hypothesized that chromatin-modifying agents (CMAs) targeting chromatin acetylation and DNA methylation could alter the chromatin configuration and turn them more amenable to reprogramming. Thus, bovine fibroblasts were treated with 5-aza-2'-deoxycytidine (AZA) plus trichostatin (TSA) or hydralazine (HH) plus valproic acid (VPA) whereas, in another trial, cloned bovine zygotes were treated with TSA. The treatment of fibroblasts with either AZA + TSA or HH + VPA increased histone acetylation, but did not affect the level of DNA methylation. However, treatment with HH + VPA decreased cellular viability and proliferation. The use of these cells as nuclear donors showed no positive effect on pre- and postimplantation development. Regarding the treatment of cloned zygotes with TSA, treated one-cell embryos showed an increase in the acetylation patterns, but not in the level of DNA methylation. Moreover, this treatment revealed no positive effect on pre- and postimplantation development. This work provides evidence the treatment of either nuclear donor cells or cloned zygotes with CMAs has no positive effect on pre- and postimplantation development of cloned cattle.
机译:尽管体细胞核移植(SCNT)是一种有前途的工具,但其潜在用途受到克隆后代发育期间高死亡率的阻碍。 SCNT后供体核的表观遗传异常编程被认为是效率低下的主要原因。我们假设针对染色质乙酰化和DNA甲基化的染色质修饰剂(CMA)可以改变染色质构型并使它们更易于重编程。因此,用5-氮杂-2'-脱氧胞苷(AZA)加曲古抑素(TSA)或肼苯哒嗪(HH)加丙戊酸(VPA)处理牛成纤维细胞,而在另一项试验中,用TSA处理克隆的牛合子。用AZA + TSA或HH + VPA处理成纤维细胞可增加组蛋白乙酰化,但不影响DNA甲基化水平。但是,用HH + VPA治疗会降低细胞活力和增殖。这些细胞用作核供体对植入前和植入后的发育没有积极影响。关于用TSA处理克隆的受精卵,处理过的单细胞胚胎显示乙酰化模式增加,但DNA甲基化水平没有增加。而且,这种治疗对植入前和植入后的发育没有积极影响。这项工作提供了用CMA处理核供体细胞或克隆受精卵的证据,对克隆牛的植入前后均无积极影响。

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