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Evidence for core exosome independent function of the nuclear exoribonuclease Rrp6p

机译:核外核糖核酸酶Rrp6p的核心外泌体独立功能的证据

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The RNA exosome processes and degrades RNAs in archaeal and eukaryotic cells. Exosomes from yeast and humans contain two active exoribonuclease components, Rrp6p and Dis3p/Rrp44p. Rrp6p is concentrated in the nucleus and the dependence of its function on the nine-subunit core exosome and Dis3p remains unclear. We found that cells lacking Rrp6p accumulate poly(A)+ rRNA degradation intermediates distinct from those found in cells depleted of Dis3p, or the core exosome component Rrp43p. Depletion of Dis3p in the absence of Rrp6p causes a synergistic increase in the levels of degradation substrates common to the core exosome and Rrp6p, but has no effect on Rrp6p-specific substrates. Rrp6p lacking a portion of its C-terminal domain no longer co-purifies with the core exosome, but continues to carry out RNA 3'-end processing of 5.8S rRNA and snoRNAs, as well as the degradation of certain truncated Rrp6-specific rRNA intermediates. However, disruption of Rrp6p-core exosome interaction results in the inability of the cell to efficiently degrade certain poly(A)+ rRNA processing products that require the combined activities of Dis3p and Rrp6p. These findings indicate that Rrp6p may carry out some of its critical functions without physical association with the core exosome.
机译:RNA外泌体加工并降解古细菌和真核细胞中的RNA。来自酵母和人类的外泌体包含两个活性的外切核糖核酸酶成分,Rrp6p和Dis3p / Rrp44p。 Rrp6p集中在细胞核中,其功能对九个亚基核心外泌体和Dis3p的依赖性仍然不清楚。我们发现缺少Rrp6p的细胞会积聚poly(A)+ rRNA降解中间体,这与在耗竭Dis3p或核心外来体成分Rrp43p的细胞中发现的中间体不同。在不存在Rrp6p的情况下耗竭Dis3p会导致核心外来体和Rrp6p共有的降解底物水平协同增加,但对Rrp6p特异性底物没有影响。缺少一部分C末端结构域的Rrp6p不再与核心外泌体共纯化,而是继续进行5.8S rRNA和snoRNA的RNA 3'末端加工,以及某些截短的Rrp6特异性rRNA的降解中间体。但是,Rrp6p-核心外来体相互作用的破坏导致细胞无法有效降解某些需要Dis3p和Rrp6p结合活性的poly(A)+ rRNA加工产物。这些发现表明,Rrp6p可能在不与核心外泌体发生物理联系的情况下执行其某些关键功能。

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