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核输出因子 RBM15 促进 DBP5 与 mRNA 的结合。

Nuclear export factor RBM15 facilitates the access of DBP5 to mRNA.

机构信息

Human Retrovirus Pathogenesis Section, National Cancer Institute-Frederick, Frederick, MD 21702-1201, USA.

出版信息

Nucleic Acids Res. 2009 Nov;37(21):7151-62. doi: 10.1093/nar/gkp782.

Abstract

The conserved mRNA export receptor NXF1 (Mex67 in yeast) assembles with messenger ribonucleoproteins (mRNP) in the nucleus and guides them through the nuclear pore complex into the cytoplasm. The DEAD family RNA helicase Dbp5 is essential for nuclear export of mRNA and is thought to dissociate Mex67 from mRNP upon translocation, thereby generating directional passage. However, the molecular mechanism by which Dbp5 recognizes Mex67-containing mRNP is not clear. Here we report that the human NXF1-binding protein RBM15 binds specifically to human DBP5 and facilitates its direct contact with mRNA in vivo. We found that RBM15 is targeted to the nuclear envelope, where it colocalizes extensively with DBP5 and NXF1. Gene silencing of RBM15 leads to cytoplasmic depletion and nuclear accumulation of general mRNA as well as individual endogenous transcripts, indicating that RBM15 is required for efficient mRNA export. We propose a model in which RBM15 acts locally at the nuclear pore complex, by facilitating the recognition of NXF1-mRNP complexes by DBP5 during translocation, thereby contributing to efficient mRNA export.

摘要

保守的 mRNA 输出受体 NXF1(酵母中的 Mex67)在核内与信使核糖核蛋白(mRNP)组装,并引导它们穿过核孔复合物进入细胞质。DEAD 家族 RNA 解旋酶 Dbp5 对于 mRNA 的核输出是必不可少的,并且被认为在易位时将 Mex67 从 mRNP 上解离,从而产生定向通道。然而,Dbp5 识别含 Mex67 的 mRNP 的分子机制尚不清楚。在这里,我们报告说,人 NXF1 结合蛋白 RBM15 特异性结合人 DBP5,并促进其在体内与 mRNA 的直接接触。我们发现 RBM15 靶向核膜,在核膜中它与 DBP5 和 NXF1 广泛共定位。RBM15 的基因沉默导致细胞质耗竭和核内积累一般 mRNA 以及个别内源性转录物,表明 RBM15 是有效 mRNA 输出所必需的。我们提出了一个模型,即 RBM15 在核孔复合物处局部起作用,通过促进 DBP5 在易位过程中识别 NXF1-mRNP 复合物,从而有助于有效的 mRNA 输出。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/38aa/2790900/4b715d0dbd47/gkp782f1.jpg

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