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屏障自整合因子的核定位与人类细胞中S期的进程相关。

Nuclear localization of barrier-to-autointegration factor is correlated with progression of S phase in human cells.

作者信息

Haraguchi Tokuko, Koujin Takako, Osakada Hiroko, Kojidani Tomoko, Mori Chie, Masuda Hirohisa, Hiraoka Yasushi

机构信息

CREST Research Project, Kansai Advanced Research Center, National Institute of Information and Communications Technology, 588-2 Iwaoka, Iwaoka-cho, Nishi-ku, Kobe 651-2492, Japan.

出版信息

J Cell Sci. 2007 Jun 15;120(Pt 12):1967-77. doi: 10.1242/jcs.03461. Epub 2007 May 22.

DOI:10.1242/jcs.03461
PMID:17519288
Abstract

Barrier-to-autointegration factor (BAF) is a conserved metazoan protein that plays a critical role in retrovirus infection. To elucidate its role in uninfected cells, we first examined the localization of BAF in both mortal and immortal or cancerous human cell lines. In mortal cell lines (e.g. TIG-1, WI-38 and IMR-90 cells) BAF localization depended on the age of the cell, localizing primarily in the nucleus of >90% of young proliferating cells but only 20-25% of aged senescent cells. In immortal cell lines (e.g. HeLa, SiHa and HT1080 cells) BAF showed heterogeneous localization between the nucleus and cytoplasm. This heterogeneity was lost when the cells were synchronized in S phase. In S-phase-synchronized populations, the percentage of cells with predominantly nuclear BAF increased from 30% (asynchronous controls) to approximately 80%. In HeLa cells, RNAi-induced downregulation of BAF significantly increased the proportion of early S-phase cells that retained high levels of cyclin D3 and cyclin E expression and slowed progression through early S phase. BAF downregulation also caused lamin A to mislocalize away from the nuclear envelope. These results indicate that BAF is required for the integrity of the nuclear lamina and normal progression of S phase in human cells.

摘要

屏障自整合因子(BAF)是一种在多细胞动物中保守的蛋白质,在逆转录病毒感染中起关键作用。为了阐明其在未感染细胞中的作用,我们首先检测了BAF在人类正常细胞系以及永生化或癌细胞系中的定位。在正常细胞系(如TIG-1、WI-38和IMR-90细胞)中,BAF的定位取决于细胞的年龄,主要定位于90%以上年轻增殖细胞的细胞核中,但仅定位于20-25%衰老细胞的细胞核中。在永生化细胞系(如HeLa、SiHa和HT1080细胞)中,BAF在细胞核和细胞质之间表现出异质性定位。当细胞在S期同步化时,这种异质性消失。在S期同步化群体中,主要定位于细胞核的BAF的细胞百分比从30%(异步对照)增加到约80%。在HeLa细胞中,RNAi诱导的BAF下调显著增加了保留高水平细胞周期蛋白D3和细胞周期蛋白E表达的早期S期细胞的比例,并减缓了通过早期S期的进程。BAF下调还导致核纤层蛋白A从核膜错位。这些结果表明,BAF是人类细胞核纤层完整性和S期正常进程所必需的。

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