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Human Ku70/80 interacts directly with hTR the RNA component of human telomerase

机译:人类Ku70 / 80与人类端粒酶的RNA成分hTR直接相互作用

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摘要

Maintenance of telomere integrity requires the dynamic interplay between telomerase, telomere-associated proteins and DNA repair proteins. These interactions are vital to suppress DNA damage responses and changes in chromosome dynamics that can result in aneuploidy or other transforming aberrations. The interaction between the DNA repair protein Ku and the RNA component of telomerase (TLC1) in Saccharomyces cerevisiae has been shown to be important for maintaining telomere length. Here, we sought to determine whether this interaction was conserved in higher eukaryotes. Although there is no sequence similarity between TLC1 and the RNA component (hTR) of human telomerase, we show that human Ku70/80 interacts with hTR both in vitro and in a cellular context. Specifically, Ku70/80 interacts with a 47 nt region of the 3′ end of hTR, which resembles the stem–loop region of the yeast Ku70/80 binding domain on TLC1. Furthermore, utilizing immunoprecipitation/RT–PCR experiments, we show that Ku interacts with hTR in cell lines deficient in the human telomerase reverse transcriptase protein (hTERT), suggesting that this interaction does not require hTERT. These data suggest that Ku interacts directly with hTR, independent of hTERT, providing evidence for the conservation of the interaction between Ku and telomerase RNA among various species and provide significant insight into how Ku is involved in telomere maintenance in higher eukaryotes.
机译:维持端粒完整性需要端粒酶,端粒相关蛋白和DNA修复蛋白之间的动态相互作用。这些相互作用对于抑制DNA损伤反应和可能导致非整倍性或其他转化畸变的染色体动力学变化至关重要。 DNA修复蛋白Ku和酿酒酵母中端粒酶(TLC1)的RNA成分之间的相互作用已被证明对于维持端粒的长度很重要。在这里,我们试图确定这种相互作用在高等真核生物中是否保守。虽然TLC1和人类端粒酶的RNA组分(hTR)之间没有序列相似性,但我们显示人Ku70 / 80在体外和细胞环境中均与hTR相互作用。特别是,Ku70 / 80与hTR 3'末端的47 nt区域相互作用,这类似于TLC1上酵母Ku70 / 80结合域的茎-环区域。此外,利用免疫沉淀/ RT-PCR实验,我们显示Ku与人类端粒酶逆转录酶蛋白(hTERT)缺乏的细胞系中的hTR相互作用,表明这种相互作用不需要hTERT。这些数据表明,Ku与hTR直接相互作用,独立于hTERT,为各种物种之间的Ku和端粒酶RNA相互作用的保守提供了证据,并提供了关于Ku如何参与高等真核生物端粒维持的重要见解。

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