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Telomere elongation involves intra-molecular DNA replication in cells utilizing alternative lengthening of telomeres

机译:端粒延长涉及利用端粒的替代延长来在细胞内进行分子内DNA复制

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Alternative lengthening of telomeres (ALT) is a telomere length maintenance mechanism based on recombination, where telomeres use other telomeric DNA as a template for DNA synthesis. About 10% of all human tumors depend on ALT for their continued growth, and understanding its molecular details is critically important for the development of cancer treatments that target this mechanism. We have previously shown that telomeres of ALT-positive human cells can become lengthened via inter-telomeric copying, i.e. by copying the telomere of another chromosome. The possibility that such telomeres could elongate by using other sources of telomeric DNA as copy templates has not been investigated previously. In this study, we have determined whether a telomere can become lengthened by copying its own sequences, without the need for using another telomere as a copy template. To test this, we transduced an ALT cell line with a telomere-targeting construct and obtained clones with a single tagged telomere. We showed that the telomere tag can be amplified without the involvement of other telomeres, indicating that telomere elongation can also occur by intra-telomeric DNA copying. This is the first direct evidence that the ALT mechanism involves more than one method of telomere elongation.
机译:端粒的替代性延长(ALT)是基于重组的端粒长度维持机制,其中端粒使用其他端粒DNA作为DNA合成的模板。所有人类肿瘤中约有10%依赖于ALT才能持续生长,因此了解其分子细节对于开发针对该机制的癌症治疗至关重要。先前我们已经表明,ALT阳性人细胞的端粒可以通过端粒间复制,即通过复制另一条染色体的端粒而变长。以前尚未研究过通过使用其他端粒DNA来源作为复制模板来延长此类端粒的可能性。在这项研究中,我们确定了是否可以通过复制自己的序列来延长端粒,而无需使用其他端粒作为复制模板。为了测试这一点,我们用靶向端粒的构建体转导了ALT细胞系,并获得了带有单个标记端粒的克隆。我们表明,端粒标签可以被扩增而无需其他端粒的参与,这表明端粒延长也可以通过端粒内DNA复制而发生。这是第一个直接证据,表明ALT机制涉及一种以上的端粒延长方法。

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