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Telomere instability in the male germline.

机译:雄性种系中的端粒不稳定。

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摘要

Telomeres play a key role in upholding the integrity of the genome, and telomerase expression in spermatogonial stem cells is responsible for the maintenance of telomere length in the human male germline. We have previously described extensive allelic variation in somatic cell telomere length that is set in the zygote, the ultimate source of which may be the germline. This implies that despite telomerase activity, substantial telomere length variation can be generated and tolerated in the germline; in order to investigate this further, we have examined the nature of telomere length variation in the human male germline. Here, we describe an analysis of both genome-wide telomere length and single molecule analysis of specific chromosome ends in human sperm. We observed individual specific differences in genome-wide telomere length. This variation may result from genetic differences within the components that determine the telomere length setting of each individual. Superimposed on the genome wide telomere length setting was a stochastic component of variation that generates germ-cells containing severely truncated telomeres. If not re-lengthened during early embryogenesis, such telomeres may limit the replicative capacity of cells derived from the zygote and have the potential to create fusagenic chromosomes, unbalanced translocations and terminal micro-deletions. These data may have implications for the genetic determination of ageing, genetic disease and fertility.
机译:端粒在维持基因组完整性方面起着关键作用,而精原干细胞中端粒酶的表达负责维持人类雄性种系中端粒的长度。先前我们已经描述了合子中体细胞端粒长度的广泛等位基因变异,其最终来源可能是种系。这意味着尽管端粒酶具有活性,但在种系中仍会产生并耐受大量的端粒长度变化。为了进一步研究,我们研究了人类雄性种系中端粒长度变异的性质。在这里,我们描述了全基因组端粒长度的分析和人类精子中特定染色体末端的单分子分析。我们观察到全基因组端粒长度的个体特异性差异。这种变化可能是由决定每个个体端粒长度设置的组件内的遗传差异引起的。叠加在基因组范围的端粒长度设置上的是变化的随机成分,该变异产生包含严重截短的端粒的生殖细胞。如果在早期胚胎发生过程中没有重新延长,这种端粒可能会限制合子细胞的复制能力,并有可能产生融合染色体,不平衡易位和末端微缺失。这些数据可能对年龄,遗传疾病和生育力的遗传测定有影响。

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