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Y 盒结合蛋白相关酸性蛋白(YBAP1/C1QBP)影响 YB-1 的定位和细胞质功能。

Y-box protein-associated acidic protein (YBAP1/C1QBP) affects the localization and cytoplasmic functions of YB-1.

机构信息

Chemical Genomics Research Group, RIKEN Center for Sustainable Resource Science, RIKEN, Wako, Saitama, Japan.

PRESTO, Japan Science and Technology Agency, Kawaguchi, Saitama, Japan.

出版信息

Sci Rep. 2018 Apr 18;8(1):6198. doi: 10.1038/s41598-018-24401-3.

Abstract

The Y-box proteins are multifunctional nucleic acid-binding proteins involved in various aspects of gene regulation. The founding member of the Y-box protein family, YB-1, functions as a transcription factor as well as a principal component of messenger ribonucleoprotein particles (mRNPs) in somatic cells. The nuclear level of YB-1 is well correlated with poor prognosis in many human cancers. Previously, we showed that a Y-box protein-associated acidic protein, YBAP1, which is identical to complement component 1, q subcomponent-binding protein (C1QBP, also called gC1qR, hyaluronan-binding protein 1 [HABP1] or ASF/SF2-associated protein p32), relieves translational repression by YB-1. Here we show that the nuclear localization of YB-1 harboring a point mutation in the cold shock domain was inhibited when co-expressed with YBAP1, whereas cytoplasmic accumulation of the wild-type YB-1 was not affected. We showed that YBAP1 inhibited the interaction between YB-1 and transportin 1. In the cytoplasm, YBAP1 affected the accumulation of YB-1 to processing bodies (P-bodies) and partially abrogated the mRNA stabilization by YB-1. Our results, indicating that YBAP1/C1QBP regulates the nucleo-cytoplasmic distribution of YB-1 and its cytoplasmic functions, are consistent with a model that YBAP1/C1QBP acts as an mRNP remodeling factor.

摘要

Y 盒蛋白是一种多功能核酸结合蛋白,参与基因调控的各个方面。Y 盒蛋白家族的创始成员 YB-1 作为转录因子以及体细胞中信使核糖核蛋白颗粒(mRNPs)的主要成分发挥作用。YB-1 的核水平与许多人类癌症的预后不良密切相关。以前,我们表明 Y 盒蛋白相关酸性蛋白 YBAP1(与补体成分 1、q 亚基结合蛋白(C1QBP,也称为 gC1qR、透明质酸结合蛋白 1 [HABP1] 或 ASF/SF2 相关蛋白 p32)相同)通过 YB-1 缓解翻译抑制。在这里,我们表明与冷休克结构域中的点突变共存时,YB-1 的核定位被抑制,而野生型 YB-1 的细胞质积累不受影响。我们表明 YBAP1 抑制 YB-1 与转运蛋白 1 之间的相互作用。在细胞质中,YBAP1 影响 YB-1 到处理体(P 体)的积累,并部分消除 YB-1 稳定 mRNA 的作用。我们的结果表明,YBAP1/C1QBP 调节 YB-1 的核质分布及其细胞质功能,与 YBAP1/C1QBP 作为 mRNP 重塑因子的模型一致。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1366/5906478/908fbeeecc48/41598_2018_24401_Fig1_HTML.jpg

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