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端粒酶逆转录酶是人类癌细胞中端粒酶RNA定位于卡哈尔体和端粒所必需的。

Telomerase reverse transcriptase is required for the localization of telomerase RNA to cajal bodies and telomeres in human cancer cells.

作者信息

Tomlinson Rebecca L, Abreu Eladio B, Ziegler Tania, Ly Hinh, Counter Christopher M, Terns Rebecca M, Terns Michael P

机构信息

Department of Biochemistry and Molecular Biology, University of Georgia, Athens, GA 30602, USA.

出版信息

Mol Biol Cell. 2008 Sep;19(9):3793-800. doi: 10.1091/mbc.e08-02-0184. Epub 2008 Jun 18.

Abstract

Telomere maintenance by telomerase is critical for the unlimited division potential of most human cancer cells. The two essential components of human telomerase, telomerase RNA (hTR) and telomerase reverse transcriptase (hTERT), are recruited from distinct subnuclear sites to telomeres during S phase. Throughout the remainder of the cell cycle hTR is found primarily in Cajal bodies. The localization of hTR to Cajal bodies and telomeres is specific to cancer cells where telomerase is active and is not observed in primary cells. Here we show that the trafficking of hTR to both telomeres and Cajal bodies depends on hTERT. RNA interference-mediated depletion of hTERT in cancer cells leads to loss of hTR from both Cajal bodies and telomeres without affecting hTR levels. In addition, expression of hTERT in telomerase-negative cells (including primary and ALT cancer cell lines) induces hTR to localize to both sites. Factors that did not stimulate hTR localization in our experiments include increased hTR RNA levels and Cajal body numbers, and expression of SV40 large T antigen and oncogenic Ras. Our findings suggest that the trafficking of telomerase to Cajal bodies and telomeres in cancer cells correlates with and depends on the assembly of the enzyme.

摘要

端粒酶对端粒的维持对于大多数人类癌细胞的无限分裂潜能至关重要。人类端粒酶的两个关键组分,端粒酶RNA(hTR)和端粒酶逆转录酶(hTERT),在S期从不同的核内亚位点被募集到端粒。在细胞周期的其余阶段,hTR主要存在于卡哈尔体中。hTR在卡哈尔体和端粒的定位是端粒酶活跃的癌细胞所特有的,在原代细胞中未观察到。在这里,我们表明hTR向端粒和卡哈尔体的运输依赖于hTERT。RNA干扰介导的癌细胞中hTERT的缺失导致hTR从卡哈尔体和端粒中丢失,而不影响hTR水平。此外,在端粒酶阴性细胞(包括原代和ALT癌细胞系)中hTERT的表达诱导hTR定位于这两个位点。在我们的实验中,未刺激hTR定位的因素包括hTR RNA水平的增加、卡哈尔体数量的增加以及SV40大T抗原和致癌性Ras的表达。我们的研究结果表明,癌细胞中端粒酶向卡哈尔体和端粒的运输与该酶的组装相关并依赖于其组装。

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