首页> 美国卫生研究院文献>Biology of Reproduction >Proteasomal Activity Is Required to Initiate and to Sustain Translational Activation of Messenger RNA Encoding the Stem-Loop-Binding Protein During Meiotic Maturation in Mice
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Proteasomal Activity Is Required to Initiate and to Sustain Translational Activation of Messenger RNA Encoding the Stem-Loop-Binding Protein During Meiotic Maturation in Mice

机译:需要蛋白酶体活性来启动和维持小鼠减数分裂成熟期间编码茎环结合蛋白的信使RNA的翻译激活。

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摘要

Developmentally regulated translation plays a key role in controlling gene expression during oogenesis. In particular, numerous mRNA species are translationally repressed in growing oocytes and become translationally activated during meiotic maturation. While many studies have focused on a U-rich sequence, termed the cytoplasmic polyadenylation element (CPE), located in the 3′-untranslated region (UTR) and the CPE-binding protein (CPEB) 1, multiple mechanisms likely contribute to translational control in oocytes. The stem-loop-binding protein (SLBP) is expressed in growing oocytes, where it is required for the accumulation of nonpolyadenylated histone mRNAs, and then accumulates substantially during meiotic maturation. We report that, in immature oocytes, Slbp mRNA carries a short poly(A) tail, and is weakly translated, and that a CPE-like sequence in the 3′-UTR is required to maintain this low activity. During maturation, Slbp mRNA becomes polyadenylated and translationally activated. Unexpectedly, proteasomal activity is required both to initiate and to sustain translational activation. This proteasomal activity is not required for the polyadenylation of Slbp mRNA during early maturation; however, it is required for a subsequent deadenylation of the mRNA that occurs during late maturation. Moreover, although CPEB1 is degraded during maturation, inhibiting its degradation by blocking mitogen-activated protein kinase 1/3 activity does not prevent the accumulation of SLBP, indicating that CPEB1 is not the protein whose degradation is required for translational activation of Slbp mRNA. These results identify a new role for proteasomal activity in initiating and sustaining translational activation during meiotic maturation.
机译:在卵子发生过程中,发育调控的翻译在控制基因表达中起关键作用。特别是,许多mRNA物种在生长的卵母细胞中被翻译抑制,并在减数分裂成熟期间被翻译激活。虽然许多研究都集中在位于3'非翻译区(UTR)和CPE结合蛋白(CPEB)1上的称为U的富含胞质的聚腺苷酸化元件(CPE)序列,但多种机制可能有助于翻译控制在卵母细胞中。茎环结合蛋白(SLBP)在生长的卵母细胞中表达,该蛋白是非聚腺苷酸组蛋白mRNA积累所必需的,然后在减数分裂成熟过程中大量积累。我们报道,在未成熟的卵母细胞中,Slbp mRNA携带一条短的poly(A)尾巴,并且翻译较弱,并且需要3'-UTR中的CPE样序列来维持这种低活性。在成熟过程中,Slbp mRNA变成聚腺苷酸化并被翻译激活。出乎意料的是,需要蛋白酶体活性来启动和维持翻译激活。早期成熟过程中,Slbp mRNA的聚腺苷酸化不需要这种蛋白酶体活性。但是,需要在后期成熟过程中进行后续的mRNA的去烯基化。而且,尽管CPEB1在成熟过程中被降解,但是通过阻断丝裂原活化的蛋白激酶1/3的活性来抑制其降解并不能阻止SLBP的积累,这表明CPEB1不是其降解是Slbp mRNA翻译激活所必需的蛋白。这些结果确定了蛋白酶体活性在减数分裂成熟期间起始和维持翻译活化中的新作用。

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