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首页> 外文期刊>Developmental biology >TRANSIENT EXPRESSION OF TRANSLATION INITIATION FACTOR EIF-4C DURING THE 2-CELL STAGE OF THE PREIMPLANTATION MOUSE EMBRYO - IDENTIFICATION BY MRNA DIFFERENTIAL DISPLAY AND THE ROLE OF DNA REPLICATION IN ZYGOTIC GENE ACTIVATION
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TRANSIENT EXPRESSION OF TRANSLATION INITIATION FACTOR EIF-4C DURING THE 2-CELL STAGE OF THE PREIMPLANTATION MOUSE EMBRYO - IDENTIFICATION BY MRNA DIFFERENTIAL DISPLAY AND THE ROLE OF DNA REPLICATION IN ZYGOTIC GENE ACTIVATION

机译:MRNA差异显示鉴定胚胎植入胚胎2期细胞转化起始因子EIF-4C的瞬时表达及其在复合基因激活中的作用。

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Zygotic gene activation (ZGA) definitely occurs by the 2-cell stage in the mouse embryo. Analysis of protein synthesis by two-dimensional gel electrophoresis reveals a class of genes whose expression transiently increases in the 2-cell embryo. Although the paucity of biological material has prevented a systematic identification of these genes, the mRNA differential display method circumvents this problem. Using this approach we find a transient increase in the mRNA abundance of the translation initiation factor eIF-4C that is inhibited by alpha-amanitin and correlated with a transient increase in the relative rate of protein synthesis for eIF-4C. We confirm the transient increase in eIF-4C mRNA abundance by a reverse transcription-PCR-based assay using eIF-4C-specific primers. The first round of DNA replication seems critical for eIF-4C expression, since addition of aphidicolin prior to S phase in the 1-cell embryo inhibits the magnitude of the increase in eIF-4C expression. Aphidicolin treatment also inhibits the synthesis of an accepted marker for ZGA, the transcription-requiring complex (TRC), which is also transiently expressed during the 2-cell stage. Incubating late 1-cell/early 2-cell embryos in medium containing aphidicolin reveals that the second round of DNA replication is not required for the increase in eIF-4C expression but DNA replication is required for the decrease in both eIF-4C expression and TRC synthesis. The decrease in eIF-4C expression, however, does not require cytokinesis or mitosis, since it occurs when 2-cell embryos are cultured in the presence of cytochalasin D or nocodazole, respectively. Changes in chromatin structure may be involved in the decrease in both eIF-4C and TRC expression, since neither decrease occurs when 2-cell embryos are cultured in trapoxin, which is a specific and irreversible inhibitor of histone deacetylase. Results of these experiments suggest that the first round of DNA replication is permissive with respect to ZGA and that the second round is repressive. (C) 1996 Academic Press, Inc. [References: 60]
机译:合子基因激活(ZGA)肯定在小鼠胚胎的2细胞阶段发生。通过二维凝胶电泳对蛋白质合成进行分析,发现了一类在2细胞胚胎中表达瞬时增加的基因。尽管生物材料的匮乏阻止了对这些基因的系统鉴定,但是mRNA差异显示方法却可以解决这个问题。使用这种方法,我们发现翻译起始因子eIF-4C的mRNA丰度出现了瞬时增加,该增加被α-amanitin抑制,并与eIF-4C蛋白质合成相对速率的瞬时增加相关。我们通过使用eIF-4C特异性引物的基于逆转录PCR的测定法确认eIF-4C mRNA的瞬时增加。 DNA复制的第一轮似乎对于eIF-4C表达至关重要,因为在1细胞胚胎的S期之前添加蚜虫可抑制eIF-4C表达增加的幅度。蚜虫碱处理还抑制了ZGA的公认标记物的合成,ZGA是需要转录的复合物(TRC),它也在2细胞阶段中瞬时表达。在含有蚜虫素的培养基中孵育晚期1细胞/早期2细胞胚胎表明,第二轮DNA复制对于eIF-4C表达的增加不是必需的,但是DNA复制对于eIF-4C表达和TRC的减少都是必需的合成。但是,eIF-4C表达的降低不需要胞质分裂或有丝分裂,因为它是在分别在细胞松弛素D或诺考达唑存在下培养2细胞胚胎时发生的。染色质结构的变化可能与eIF-4C和TRC表达的降低有关,因为当2细胞胚胎在作为组蛋白脱乙酰基酶的一种特异性且不可逆的抑制剂trapoxin中培养时,这两种降低都不会发生。这些实验的结果表明,相对于ZGA,第一轮DNA复制是允许的,而第二轮是抑制性的。 (C)1996 Academic Press,Inc. [参考:60]

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