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首页> 外文期刊>Molecular and Cellular Biology >CstF64: Cell Cycle Regulation and Functional Role in 3′ End Processing of Replication-Dependent Histone mRNAs
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CstF64: Cell Cycle Regulation and Functional Role in 3′ End Processing of Replication-Dependent Histone mRNAs

机译:CstF64:复制依赖的组蛋白mRNA的3'末端加工中的细胞周期调控和功能作用

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摘要

The 3′ end processing of animal replication-dependent histone mRNAs is activated during G1/S-phase transition. The processing site is recognized by stem-loop binding protein and the U7 snRNP, but cleavage additionally requires a heat-labile factor (HLF), composed of cleavage/polyadenylation specificity factor, symplekin, and cleavage stimulation factor 64 (CstF64). Although HLF has been shown to be cell cycle regulated, the mechanism of this regulation is unknown. Here we show that levels of CstF64 increase toward the S phase and its depletion affects histone RNA processing, S-phase progression, and cell proliferation. Moreover, analyses of the interactions between CstF64, symplekin, and the U7 snRNP-associated proteins FLASH and Lsm11 indicate that CstF64 is important for recruiting HLF to histone precursor mRNA (pre-mRNA)-resident proteins. Thus, CstF64 is central to the function of HLF and appears to be at least partly responsible for its cell cycle regulation. Additionally, we show that misprocessed histone transcripts generated upon CstF64 depletion mainly accumulate in the nucleus, where they are targets of the exosome machinery, while a small cytoplasmic fraction is partly associated with polysomes.
机译:动物复制依赖性组蛋白mRNA的3'末端加工在G 1 / S期转变过程中被激活。加工位点被茎环结合蛋白和U7 snRNP识别,但裂解还需要一个热不稳定因子(HLF),该因子由裂解/聚腺苷酸特异性因子,辛普金和裂解刺激因子64(CstF64)组成。尽管已显示HLF受细胞周期调节,但这种调节的机制尚不清楚。在这里,我们显示CstF64的水平朝S期增加,其消耗会影响组蛋白RNA加工,S期进程和细胞增殖。此外,对CstF64,symplekin和U7 snRNP相关蛋白FLASH和Lsm11之间的相互作用的分析表明,CstF64对于将HLF募集到组蛋白前体mRNA(pre-mRNA)驻留蛋白很重要。因此,CstF64对HLF的功能至关重要,并且似乎至少部分负责其细胞周期调节。此外,我们显示CstF64耗尽后产生的处理不当的组蛋白转录本主要聚集在核中,它们是外泌体机制的靶标,而一小部分细胞质与多核糖体相关。

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