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前体 mRNA 滞留和剪接复合物控制着中介体亚基 Med20 的表达。

The pre-mRNA retention and splicing complex controls expression of the Mediator subunit Med20.

机构信息

a Department of Molecular Biology , Umeå University , Umeå , Sweden.

b BRF Krutet , Norra Majorsgatan, Umeå , Sweden.

出版信息

RNA Biol. 2017 Oct 3;14(10):1411-1417. doi: 10.1080/15476286.2017.1294310. Epub 2017 Feb 17.

Abstract

The heterotrimeric pre-mRNA retention and splicing (RES) complex, consisting of Bud13p, Snu17p and Pml1p, promotes splicing and nuclear retention of a subset of intron-containing pre-mRNAs. Yeast cells deleted for individual RES genes show growth defects that are exacerbated at elevated temperatures. Although the growth phenotypes correlate to the splicing defects in the individual mutants, the underlying mechanism is unknown. Here, we show that the temperature sensitive (Ts) growth phenotype of bud13Δ and snu17Δ cells is a consequence of inefficient splicing of MED20 pre-mRNA, which codes for a subunit of the Mediator complex; a co-regulator of RNA polymerase II transcription. The MED20 pre-mRNA splicing defect is less pronounced in pml1Δ cells, explaining why they grow better than the other 2 RES mutants at elevated temperatures. Inactivation of the cytoplasmic nonsense-mediated mRNA decay (NMD) pathway in the RES mutants leads to accumulation of MED20 pre-mRNA, indicating that inefficient nuclear retention contributes to the growth defect. Further, the Ts phenotype of bud13Δ and snu17Δ cells is partially suppressed by the inactivation of NMD, showing that the growth defects are augmented by the presence of a functional NMD pathway. Collectively, our results demonstrate an important role of the RES complex in maintaining the Med20p levels.

摘要

三聚体前体 mRNA 滞留和剪接 (RES) 复合物由 Bud13p、Snu17p 和 Pml1p 组成,促进了一组内含子前体 mRNA 的剪接和核滞留。酵母细胞中单个 RES 基因的缺失会导致生长缺陷,而在高温下这种缺陷会加剧。尽管单个突变体的生长表型与剪接缺陷相关,但潜在的机制尚不清楚。在这里,我们表明 bud13Δ 和 snu17Δ 细胞的温度敏感(Ts)生长表型是 MED20 前体 mRNA 剪接效率低下的结果,MED20 前体 mRNA 编码 Mediator 复合物的一个亚基;RNA 聚合酶 II 转录的共调节剂。pml1Δ 细胞中的 MED20 前体 mRNA 剪接缺陷不太明显,这解释了为什么它们在高温下比其他 2 个 RES 突变体生长得更好。在 RES 突变体中,细胞质无义介导的 mRNA 降解 (NMD) 途径的失活导致 MED20 前体 mRNA 的积累,表明核滞留效率低下导致生长缺陷。此外,NMD 的失活部分抑制了 bud13Δ 和 snu17Δ 细胞的 Ts 表型,表明存在功能正常的 NMD 途径会加剧生长缺陷。总的来说,我们的结果表明 RES 复合物在维持 Med20p 水平方面发挥着重要作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bdfc/5711472/68726820c0a0/krnb-14-10-1294310-g001.jpg

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