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茎环结合蛋白在卵母细胞成熟过程中积累,并且在小鼠早期胚胎中不受细胞周期调控。

Stem-loop binding protein accumulates during oocyte maturation and is not cell-cycle-regulated in the early mouse embryo.

作者信息

Allard Patrick, Champigny Marc J, Skoggard Sarah, Erkmann Judith A, Whitfield Michael L, Marzluff William F, Clarke Hugh J

机构信息

Department of Obstetrics and Gynecology, McGill University, Montreal, Quebec, Canada H3A 1A1.

出版信息

J Cell Sci. 2002 Dec 1;115(Pt 23):4577-86. doi: 10.1242/jcs.00132.

Abstract

The stem-loop binding protein (SLBP) binds to the 3' end of histone mRNA and participates in 3'-processing of the newly synthesized transcripts, which protects them from degradation, and probably also promotes their translation. In proliferating cells, translation of SLBP mRNA begins at G1/S and the protein is degraded following DNA replication. These post-transcriptional mechanisms closely couple SLBP expression to S-phase of the cell cycle, and play a key role in restricting synthesis of replication-dependent histones to S-phase. In contrast to somatic cells, replication-dependent histone mRNAs accumulate and are translated independently of DNA replication in oocytes and early embryos. We report here that SLBP expression and activity also differ in mouse oocytes and early embryos compared with somatic cells. SLBP is present in oocytes that are arrested at prophase of G2/M, where it is concentrated in the nucleus. Upon entry into M-phase of meiotic maturation, SLBP begins to accumulate rapidly, reaching a very high level in mature oocytes arrested at metaphase II. Following fertilization, SLBP remains abundant in the nucleus and the cytoplasm throughout the first cell cycle, including both G1 and G2 phases. It declines during the second and third cell cycles, reaching a relatively low level by the late 4-cell stage. SLBP can bind the histone mRNA-stem-loop at all stages of the cell cycle in oocytes and early embryos, and it is the only stem-loop binding activity detectable in these cells. We also report that SLBP becomes phosphorylated rapidly following entry into M-phase of meiotic maturation through a mechanism that is sensitive to roscovitine, an inhibitor of cyclin-dependent kinases. SLBP is rapidly dephosphorylated following fertilization or parthenogenetic activation, and becomes newly phosphorylated at M-phase of mitosis. Phosphorylation does not affect its stem-loop binding activity. These results establish that, in contrast to Xenopus, mouse oocytes and embryos contain a single SLBP. Expression of SLBP is uncoupled from S-phase in oocytes and early embryos, which indicates that the mechanisms that impose cell-cycle-regulated expression of SLBP in somatic cells do not operate in oocytes or during the first embryonic cell cycle. This distinctive pattern of SLBP expression may be required for accumulation of histone proteins required for sperm chromatin remodelling and assembly of newly synthesized embryonic DNA into chromatin.

摘要

茎环结合蛋白(SLBP)与组蛋白mRNA的3'端结合,并参与新合成转录本的3'加工过程,这可保护它们不被降解,还可能促进其翻译。在增殖细胞中,SLBP mRNA的翻译在G1/S期开始,蛋白质在DNA复制后被降解。这些转录后机制将SLBP的表达与细胞周期的S期紧密联系起来,并在将复制依赖型组蛋白的合成限制在S期方面发挥关键作用。与体细胞不同,复制依赖型组蛋白mRNA在卵母细胞和早期胚胎中积累并独立于DNA复制进行翻译。我们在此报告,与体细胞相比,小鼠卵母细胞和早期胚胎中的SLBP表达和活性也有所不同。SLBP存在于停滞在G2/M期前期的卵母细胞中,集中在细胞核内。进入减数分裂成熟的M期后,SLBP开始迅速积累,在停滞于中期II的成熟卵母细胞中达到非常高的水平。受精后,在整个第一个细胞周期,包括G1和G2期,SLBP在细胞核和细胞质中都保持丰富。在第二个和第三个细胞周期中它会下降,到4细胞晚期达到相对较低的水平。在卵母细胞和早期胚胎的细胞周期所有阶段,SLBP都能结合组蛋白mRNA茎环,并且它是这些细胞中唯一可检测到的茎环结合活性。我们还报告,通过对细胞周期蛋白依赖性激酶抑制剂roscovitine敏感的机制,减数分裂成熟进入M期后SLBP会迅速磷酸化。受精或孤雌激活后,SLBP会迅速去磷酸化,并在有丝分裂的M期重新磷酸化。磷酸化不影响其茎环结合活性。这些结果表明,与非洲爪蟾不同,小鼠卵母细胞和胚胎含有单一的SLBP。在卵母细胞和早期胚胎中,SLBP的表达与S期解偶联,这表明在体细胞中施加细胞周期调控SLBP表达的机制在卵母细胞或第一个胚胎细胞周期中不起作用。这种独特的SLBP表达模式可能是精子染色质重塑以及将新合成的胚胎DNA组装成染色质所需组蛋白积累所必需的。

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