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Modulation of Telomeres in Alternative Lengthening of Telomeres Type I Like Human Cells by the Expression of Werner Protein and Telomerase

机译:通过Werner蛋白和端粒酶的表达调节端粒的替代性延长I型端粒像人类细胞。

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摘要

The alternative lengthening of telomeres (ALT) is a recombination-based mechanism of telomere maintenance activated in 5–20% of human cancers. In Saccharomyces cerevisiae, survivors that arise after inactivation of telomerase can be classified as type I or type II ALT. In type I, telomeres have a tandem array structure, with each subunit consisting of a subtelomeric Y′ element and short telomere sequence. Telomeres in type II have only long telomere repeats and require Sgs1, the S. cerevisiae RecQ family helicase. We previously described the first human ALT cell line, AG11395, that has a telomere structure similar to type I ALT yeast cells. This cell line lacks the activity of the Werner syndrome protein, a human RecQ helicase. The telomeres in this cell line consist of tandem repeats containing SV40 DNA, including the origin of replication, and telomere sequence. We investigated the role of the SV40 origin of replication and the effects of Werner protein and telomerase on telomere structure and maintenance in AG11395 cells. We report that the expression of Werner protein facilitates the transition in human cells of ALT type I like telomeres to type II like telomeres in some aspects. These findings have implications for the diagnosis and treatment of cancer.
机译:端粒的替代性延长(ALT)是一种基于重组的端粒维持机制,在5-20%的人类癌症中被激活。在酿酒酵母中,端粒酶失活后出现的幸存者可分为I型或II型ALT。在I型中,端粒具有串联阵列结构,每个亚基由亚端粒Y'元件和短端粒序列组成。 II型端粒只有较长的端粒重复序列,并且需要酿酒酵母RecQ家族解旋酶Sgs1。先前我们描述了第一个人类ALT细胞系AG11395,其端粒结构与I型ALT酵母细胞相似。该细胞系缺乏Werner综合征蛋白(人类RecQ解旋酶)的活性。该细胞系中的端粒由含有SV40 DNA的串联重复序列组成,包括复制起点和端粒序列。我们调查了SV40复制起点的作用以及Werner蛋白和端粒酶对AG11395细胞端粒结构和维持的影响。我们报道,在某些方面,Werner蛋白的表达促进人类细胞中ALT型I端粒转变为II型端粒。这些发现对癌症的诊断和治疗具有重要意义。

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