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The number of vertebrate repeats can be regulated at yeast telomeres by Rap1-independent mechanisms

机译:可以通过不依赖Rap1的机制在酵母端粒上调节脊椎动物重复序列的数量

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摘要

The number of telomeric DNA repeats at chromosome ends is maintained around a mean value by a dynamic balance between elongation and shortening. In particular, proteins binding along the duplex part of telomeric DNA set the number of repeats by progressively limiting telomere growth. The paradigm of this counting mechanism is the Rap1 protein in Saccharomyces cerevisiae. We demonstrate here that a Rap1-independent mechanism regulates the number of yeast telomeric repeats (TG1–3) and of vertebrate repeats (T2AG3) when TEL1, a yeast ortholog of the human gene encoding the ATM kinase, is inactivated. In addition, we show that a T2AG3-only telomere can be formed and maintained in humanized yeast cells carrying a template mutation of the gene encoding the telomerase RNA, which leads to the synthesis of vertebrate instead of yeast repeats. Genetic and biochemical evidences indicate that this telomere is regulated in a Rap1-independent manner, both in TEL1 and in tel1Δ humanized yeast cells. Altogether, these findings shed light on multiple repeat-counting mechanisms, which may share critical features between lower and higher eukaryotes.
机译:通过延长和缩短之间的动态平衡,染色体末端的端粒DNA重复数保持在平均值附近。特别地,沿着端粒DNA的双链体部分结合的蛋白质通过逐渐限制端粒的生长来设定重复的数目。这种计数机制的范例是酿酒酵母中的Rap1蛋白。我们在这里证明,当TEL1(编码ATM激酶的人类基因的酵母直系同源物)被失活时,Rap1依赖性机制调节酵母端粒重复序列(TG1-3)和脊椎动物重复序列(T2AG3)的数量。此外,我们表明,在携带编码端粒酶RNA的基因的模板突变的人源化酵母细胞中,可以形成并维持仅T2AG3端粒,这导致脊椎动物的合成而不是酵母重复。遗传和生物化学证据表明,该端粒在TEL1和tel1Δ人源化酵母细胞中均受Rap1依赖性调控。总而言之,这些发现揭示了多种重复计数机制,这些机制可能在低等和高等真核生物之间共享关键特征。

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