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基于经典核输入及其他非经典核输入机制的“搭便车”现象在人类蛋白质组中似乎极为普遍。

Piggybacking on Classical Import and Other Non-Classical Mechanisms of Nuclear Import Appear Highly Prevalent within the Human Proteome.

作者信息

Tessier Tanner M, MacNeil Katelyn M, Mymryk Joe S

机构信息

Department of Microbiology and Immunology, The University of Western Ontario, London, ON N6A 3K7, Canada.

Department of Otolaryngology, Head & Neck Surgery, The University of Western Ontario, London, ON N6A 3K7, Canada.

出版信息

Biology (Basel). 2020 Jul 23;9(8):188. doi: 10.3390/biology9080188.

DOI:10.3390/biology9080188
PMID:32718019
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7463951/
Abstract

One of the most conserved cellular pathways among eukaryotes is the extensively studied classical protein nuclear import pathway mediated by importin-α. Classical nuclear localization signals (cNLSs) are recognized by importin-α and are highly predictable due to their abundance of basic amino acids. However, various studies in model organisms have repeatedly demonstrated that only a fraction of nuclear proteins contain identifiable cNLSs, including those that directly interact with importin-α. Using data from the Human Protein Atlas and the Human Reference Interactome, and proteomic data from BioID/protein-proximity labeling studies using multiple human importin-α proteins, we determine that nearly 50% of the human nuclear proteome does not have a predictable cNLS. Surprisingly, between 25% and 50% of previously identified human importin-α cargoes do not have predictable cNLS. Analysis of importin-α cargo without a cNLS identified an alternative basic rich motif that does not resemble a cNLS. Furthermore, several previously suspected piggybacking proteins were identified, such as those belonging to the RNA polymerase II and transcription factor II D complexes. Additionally, many components of the mediator complex interact with at least one importin-α, yet do not have a predictable cNLS, suggesting that many of the subunits may enter the nucleus through an importin-α-dependent piggybacking mechanism.

摘要

真核生物中最保守的细胞通路之一是由输入蛋白-α介导的经过广泛研究的经典蛋白质核输入通路。经典核定位信号(cNLSs)可被输入蛋白-α识别,由于其富含碱性氨基酸,所以具有高度可预测性。然而,对模式生物的各种研究反复表明,只有一小部分核蛋白含有可识别的cNLSs,包括那些直接与输入蛋白-α相互作用的蛋白。利用人类蛋白质图谱和人类参考相互作用组的数据,以及使用多种人类输入蛋白-α进行生物ID/蛋白质邻近标记研究获得的蛋白质组学数据,我们确定近50%的人类核蛋白质组没有可预测的cNLS。令人惊讶的是,先前鉴定的人类输入蛋白-α货物中有25%至50%没有可预测的cNLS。对没有cNLS的输入蛋白-α货物进行分析,发现了一种不同于cNLS的富含碱性氨基酸的基序。此外,还鉴定出了几种先前怀疑的搭载蛋白,如那些属于RNA聚合酶II和转录因子IID复合物的蛋白。另外,中介体复合物的许多成分与至少一种输入蛋白-α相互作用,但没有可预测的cNLS,这表明许多亚基可能通过依赖于输入蛋白-α的搭载机制进入细胞核。

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