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早期胚胎阶段组蛋白H3的乙酰化水平影响小型猪体细胞核移植胚胎的后续发育。

Acetylation level of histone H3 in early embryonic stages affects subsequent development of miniature pig somatic cell nuclear transfer embryos.

作者信息

Yamanaka Ken-ichi, Sugimura Satoshi, Wakai Takuya, Kawahara Manabu, Sato Eimei

机构信息

National Agricultural Research Center for Kyushu Okinawa Region (KONARC), Kumamoto, Japan.

出版信息

J Reprod Dev. 2009 Dec;55(6):638-44. doi: 10.1262/jrd.20245. Epub 2009 Aug 24.

Abstract

Successful cloning by somatic cell nuclear transfer (SCNT) requires a reprogramming process in which the epigenetic state of a differentiated donor nucleus must be converted into an embryonic totipotent state. However, this epigenetic reprogramming is incomplete in SCNT embryos, causing low production efficiency. Recently, it has been reported that trichostatin A (TSA), an inhibitor of histone deacetylase, potentially enhances cloning efficiency. The aim of the present study was to optimize the TSA treatment for miniature pig SCNT embryos and investigate the effect of the acetylation level of histone on developmental competence of SCNT embryos. In order to optimize the TSA treatment, we examined the developmental competence of SCNT embryos under various exposure times (0-50 h) and concentrations (0-500 nM). Treatment with 5 nM TSA for 15 and 20 h beginning at the start of activation significantly increased the blastocyst formation rate (34.6 and 32.4 vs. 18.2%, respectively) and mean cell number (57.0 +/- 2.7 and 56.6 +/- 2.7 vs. 43.5 +/- 2.1, respectively) as compared with the non-treated group (0 h). We then investigated the acetylation levels of histone H3 in SCNT embryos treated with or without TSA (TSA (+) or TSA (-)) as compared with in vitro- fertilized (IVF) embryos. The acetylation levels of the TSA (-) SCNT embryos at the pseudo-pronuclear and 2-cell stages were significantly lower than those of the IVF embryos at the same developmental stages. In contrast, the acetylation levels of the TSA (+) SCNT embryos were similar to those of the IVF embryos. There was no difference in the acetylation levels of all groups at the blastocyst stage. Our data therefore suggests that the acetylation level of histone H3 at the pseudo-pronuclear and 2-cell stages is positively correlated with subsequent development of SCNT embryos, which may be an important event for the vital development of SCNT embryos in miniature pigs.

摘要

通过体细胞核移植(SCNT)成功克隆需要一个重编程过程,在此过程中,分化的供体细胞核的表观遗传状态必须转化为胚胎全能状态。然而,这种表观遗传重编程在SCNT胚胎中并不完全,导致生产效率低下。最近,有报道称,组蛋白脱乙酰酶抑制剂曲古抑菌素A(TSA)可能提高克隆效率。本研究的目的是优化对小型猪SCNT胚胎的TSA处理,并研究组蛋白乙酰化水平对SCNT胚胎发育能力的影响。为了优化TSA处理,我们检测了SCNT胚胎在不同暴露时间(0 - 50小时)和浓度(0 - 500 nM)下的发育能力。从激活开始用5 nM TSA处理15和20小时,与未处理组(0小时)相比,显著提高了囊胚形成率(分别为34.6%和32.4%,而未处理组为18.2%)和平均细胞数(分别为57.0±2.7和56.6±2.7,而未处理组为43.5±2.1)。然后,我们研究了与体外受精(IVF)胚胎相比,经或未经TSA处理(TSA(+)或TSA(-))的SCNT胚胎中组蛋白H3的乙酰化水平。TSA(-)SCNT胚胎在原核和2细胞阶段的乙酰化水平显著低于相同发育阶段的IVF胚胎。相反,TSA(+)SCNT胚胎的乙酰化水平与IVF胚胎相似。所有组在囊胚阶段的乙酰化水平没有差异。因此,我们的数据表明,原核和2细胞阶段组蛋白H3的乙酰化水平与SCNT胚胎的后续发育呈正相关,这可能是小型猪SCNT胚胎重要发育过程中的一个重要事件。

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