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DNA双链断裂处端粒添加的调控。

Regulation of telomere addition at DNA double-strand breaks.

作者信息

Ribeyre Cyril, Shore David

机构信息

Department of Molecular Biology, National Center for Competence in Research NCCR program Frontiers in Genetics, University of Geneva, 30 quai Ernest-Ansermet, 1211, Geneva 4, Switzerland.

出版信息

Chromosoma. 2013 Jun;122(3):159-73. doi: 10.1007/s00412-013-0404-2. Epub 2013 Mar 17.

Abstract

Telomeres constitute the ends of linear eukaryotic chromosomes. Due to the conventional mode of DNA replication, telomeric DNA erodes at each cell division. To counteract this, a specialized reverse transcriptase, telomerase, can elongate chromosome ends to maintain them at a constant average length. Because of their similarity to DNA double-strand breaks (DSBs), telomeres might be expected to induce a DNA damage response, which would lead to repair reactions and the generation of translocations or fusions. Many proteins present at telomeres prevent this by protecting (capping) the chromosome termini. Conversely, a DSB occurring in other regions of the genome, due, for instance, to a stalled replication fork or genotoxic agents, must be repaired by homologous recombination or end-joining to ensure genome stability. Interestingly, telomerase is able to generate a telomere de novo at an accidental DSB, with potentially lethal consequences in haploid cells and, at a minimum, loss of heterozygosity (LOH) in diploid cells. Recent data suggest that telomerase is systematically recruited to DSBs but is prevented from acting in the absence of a minimal stretch of flanking telomere-repeat sequences. In this review, we will focus on the mechanisms that regulate telomere addition to DSBs.

摘要

端粒构成线性真核染色体的末端。由于DNA复制的传统模式,端粒DNA在每次细胞分裂时都会缩短。为了抵消这种情况,一种特殊的逆转录酶——端粒酶,可以延长染色体末端,使其保持在恒定的平均长度。由于端粒与DNA双链断裂(DSB)相似,可能会引发DNA损伤反应,进而导致修复反应以及易位或融合的产生。端粒上存在的许多蛋白质通过保护(封端)染色体末端来防止这种情况发生。相反,基因组其他区域发生的DSB,例如由于复制叉停滞或基因毒性剂导致的,必须通过同源重组或末端连接进行修复,以确保基因组稳定性。有趣的是,端粒酶能够在偶然出现的DSB处重新生成端粒,这在单倍体细胞中可能产生致命后果,在二倍体细胞中至少会导致杂合性丧失(LOH)。最近的数据表明,端粒酶会被系统性地招募到DSB处,但在没有最小长度的侧翼端粒重复序列时会被阻止发挥作用。在这篇综述中,我们将重点关注调控在DSB处添加端粒的机制。

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