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首页> 外文期刊>Journal of molecular cell biology >The conserved ubiquitin-like protein Hub1 plays a critical role in splicing in human cells.
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The conserved ubiquitin-like protein Hub1 plays a critical role in splicing in human cells.

机译:保守的泛素样蛋白Hub1在人细胞剪接中起关键作用。

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Different from canonical ubiquitin-like proteins, Hub1 does not form covalent conjugates with substrates but binds proteins non-covalently. In Saccharomyces cerevisiae, Hub1 associates with spliceosomes and mediates alternative splicing of SRC1, without affecting pre-mRNA splicing generally. Human Hub1 is highly similar to its yeast homolog, but its cellular function remains largely unexplored. Here, we show that human Hub1 binds to the spliceosomal protein Snu66 as in yeast; however, unlike its S. cerevisiae homolog, human Hub1 is essential for viability. Prolonged in vivo depletion of human Hub1 leads to various cellular defects, including splicing speckle abnormalities, partial nuclear retention of mRNAs, mitotic catastrophe, and consequently cell death by apoptosis. Early consequences of Hub1 depletion are severe splicing defects, however, only for specific splice sites leading to exon skipping and intron retention. Thus, the ubiquitin-like protein Hub1 is not a canonical spliceosomal factor needed generally for splicing, but rather a modulator of spliceosome performance and facilitator of alternative splicing.
机译:与典型的泛素样蛋白不同,Hub1不会与底物形成共价结合物,而是非共价结合蛋白。在酿酒酵母中,Hub1与剪接体缔合并介导SRC1的选择性剪接,而通常不会影响mRNA的剪接。人Hub1与它的酵母同源物高度相似,但其细胞功能仍未开发。在这里,我们显示人Hub1与酵母中的剪接蛋白Snu66结合。然而,与其酿酒酵母同源物不同,人类Hub1对于生存力至关重要。人Hub1在体内的长时间耗竭会导致各种细胞缺陷,包括剪接斑点异常,mRNA的部分核保留,有丝分裂灾难以及因此导致的细胞凋亡。 Hub1耗尽的早期后果是严重的剪接缺陷,但是,仅对于特定的剪接位点会导致外显子跳跃和内含子保留。因此,泛素样蛋白Hub1并不是剪接通常所需的规范剪接体因子,而是剪接体性能的调节剂和替代剪接的促进剂。

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