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FLJ25439,一种新型的胞质分裂相关蛋白,通过增强内质网应激伴侣蛋白的表达诱导四倍体化并维持染色体稳定性。

FLJ25439, a novel cytokinesis-associated protein, induces tetraploidization and maintains chromosomal stability via enhancing expression of endoplasmic reticulum stress chaperones.

作者信息

Pan Tai-Long, Hsu Shu-Yuan, Wang Pei-Wen, Cheng Ya-Ting, Chang Yu-Chen, Saha Sudipta, Hu Jiwei, Ouyang Pin

机构信息

a School of Traditional Chinese Medicine; Chang Gung University ; Taoyuan , Taiwan.

出版信息

Cell Cycle. 2015;14(8):1174-87. doi: 10.1080/15384101.2015.1010906.

DOI:10.1080/15384101.2015.1010906
PMID:25751302
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4614365/
Abstract

Investigation of the mechanisms leading to aneuploidy and polyploidy is critical to cancer research. Previous studies have provided strong evidence of the importance of tetraploidization as an early step in tumorigenesis. In cancer cells, tetraploid cells may contribute to abnormal mitotic progression, which may be associated with cytokinesis failure. Tetraploidy leads to genomic instability due to centrosome and chromosome over-replication. Until now, the mechanism by which cells maintain tetraploid status has been unknown. Here, we identified a novel D box-containing protein, FLJ25439, which displays a dynamic expression profile during mitosis/cytokinesis with the midbody as the most prominent associated structure. To understand the function of FLJ25439, we established stable cell lines overexpressing FLJ25439. FLJ25439-overexpression cells grew slower and displayed a tetraploid DNA content in comparison with diploid parental cells. They also showed aberrant mitosis and dysregulated expression of p53, pRb and p21, suggesting a defect in cell cycle progression. To explore the molecular mechanisms responsible for FLJ25439-induced tetraploidization, we conducted a comparative analysis of the global protein expression patterns of wild type and overexpressors using proteomics and bioinformatics approaches. Protein category profiling indicated that FLJ25439 is involved in pathways related to anti-apoptosis, protein folding, the cell cycle, and cytoskeleton regulation. Specifically, genotoxic-stress- and ER stress-related chaperone proteins greatly contributed to the FLJ25439 overexpression phenotypes. The results of this study pave the way to our further understanding of the role of this novel cytokinesis-related protein in protecting cells from environmental stress and tetraploid formation.

摘要

研究导致非整倍体和多倍体的机制对癌症研究至关重要。先前的研究提供了强有力的证据,证明四倍体化作为肿瘤发生早期步骤的重要性。在癌细胞中,四倍体细胞可能导致异常的有丝分裂进程,这可能与胞质分裂失败有关。四倍体由于中心体和染色体过度复制而导致基因组不稳定。到目前为止,细胞维持四倍体状态的机制尚不清楚。在这里,我们鉴定了一种新型的含D盒蛋白FLJ25439,它在有丝分裂/胞质分裂过程中呈现动态表达谱,其中间体是最突出的相关结构。为了了解FLJ25439的功能,我们建立了过表达FLJ25439的稳定细胞系。与二倍体亲本细胞相比,过表达FLJ25439的细胞生长较慢,并且显示出四倍体DNA含量。它们还表现出异常的有丝分裂以及p53、pRb和p21的表达失调,表明细胞周期进程存在缺陷。为了探索导致FLJ25439诱导四倍体化的分子机制,我们使用蛋白质组学和生物信息学方法对野生型和过表达细胞的整体蛋白质表达模式进行了比较分析。蛋白质类别分析表明,FLJ25439参与了与抗凋亡、蛋白质折叠、细胞周期和细胞骨架调节相关的途径。具体而言,与基因毒性应激和内质网应激相关的伴侣蛋白对FLJ25439过表达表型有很大贡献。这项研究的结果为我们进一步了解这种新型胞质分裂相关蛋白在保护细胞免受环境应激和四倍体形成中的作用铺平了道路。

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