首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Human POT1 disrupts telomeric G-quadruplexes allowing telomerase extension in vitro.
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Human POT1 disrupts telomeric G-quadruplexes allowing telomerase extension in vitro.

机译:人POT1破坏端粒G-四链体,允许端粒酶在体外延伸。

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摘要

The POT1 (protection of telomeres 1) protein binds the ssDNA overhangs at the ends of chromosomes in diverse eukaryotes. POT1 is essential for chromosome end-protection, as best demonstrated in fission yeast. In human cells, hPOT1 is also involved in telomere-length regulation. We now show that telomeric oligonucleotides, such as d[GGG(TTAGGG)(3)], which form intramolecular G-quadruplexes through Hoogsteen base-pairing, serve as only marginal primers for extension by recombinant human telomerase; telomerase stalls after every nucleotide addition. Addition of hPOT1 to the reaction restores the normal processive elongation pattern seen with primers that cannot form G-quadruplexes. hPOT1 does not act catalytically but, instead, forms a stoichiometric complex with the DNA, freeing its 3' tail. An antisense oligonucleotide, which base-pairs near the 5' end of the telomeric sequence, leaving a telomerase-extendable 3' tail, duplicates the effect of hPOT1 on activation of G-quadruplex primers. Thus, hPOT1 mayfunction simply by trapping the unfolded forms of these telomeric primers in an equilibrium population. We propose an additional role for hPOT1 in telomere maintenance: disrupting G-quadruplex structures in telomeric DNA, thereby allowing proper elongation by telomerase.
机译:POT1(端粒1的保护)蛋白与各种真核生物中染色体末端的ssDNA突出端结合。正如裂变酵母所充分证明的那样,POT1对于染色体末端保护至关重要。在人类细胞中,hPOT1也参与端粒长度调节。我们现在显示端粒寡核苷酸,例如通过Hoogsteen碱基配对形成分子内G-四链体的d [GGG(TTAGGG)(3)],仅用作重组人端粒酶延伸的边际引物。每次添加核苷酸后,端粒酶停顿。向反应中添加hPOT1可恢复无法形成G-四链体的引物所见的正常进行性延伸模式。 hPOT1并不起催化作用,而是与DNA形成化学计量的复合物,释放其3'尾巴。一种反义寡核苷酸,其在端粒序列的5'末端附近碱基配对,而留下一个端粒酶可延伸的3'尾巴,可复制hPOT1对G-四链体引物活化的作用。因此,hPOT1可以简单地通过将这些端粒引物的未折叠形式捕获在平衡群体中来发挥作用。我们提出hPOT1在端粒维持中的其他作用:破坏端粒DNA中的G-四链体结构,从而允许端粒酶适当延长。

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