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首页> 外文期刊>Human Molecular Genetics >Telomere length and the expression of natural telomeric genes in human fibroblasts.
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Telomere length and the expression of natural telomeric genes in human fibroblasts.

机译:人成纤维细胞中端粒的长度和天然端粒基因的表达。

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摘要

Progressive telomere shortening occurs with division of normal human cells, and eventually leads to replicative senescence. The mechanism by which the shortened telomeres cause growth arrest is largely unknown. Transcriptional silencing of genes adjacent to telomeres, also called telomere position effect, has been hypothesized as a possible mechanism of telomere-mediated senescence. However, there is no report regarding telomere position effect on natural telomeric genes in human cells. To address whether the expression of natural telomeric genes is regulated by telomere length, we combined quantitative RT-PCR with quantitative fluorescence in situ hybridization to comparatively analyze the expression of 34 telomeric genes and telomere length of their 24 corresponding chromosome ends in young and senescent human fibroblasts. We have demonstrated here that telomere length alone is not sufficient to determine the expression status of natural telomeric genes. An extended analysis of a tandem of eight telomeric genes on a single chromosome end revealed a discontinuous pattern of changed expression during telomere shortening and some of the changes are senescence-specific rather than non-dividing-related. These results suggest that the expression of natural telomeric genes may be influenced by alteration of local heterochromatin structure.
机译:渐进的端粒缩短随着正常人细胞的分裂而发生,并最终导致复制性衰老。缩短的端粒引起生长停滞的机制在很大程度上是未知的。端粒邻近基因的转录沉默(也称为端粒位置效应)被认为是端粒介导衰老的可能机制。然而,没有关于端粒位置对人细胞中天然端粒基因的影响的报道。为了探讨天然端粒基因的表达是否受端粒长度调控,我们将定量RT-PCR与定量荧光原位杂交相结合,比较分析了34个端粒基因的表达及其在24岁和衰老人类中端粒的长度。成纤维细胞。我们在这里证明了端粒长度不足以决定天然端粒基因的表达状态。扩展分析单个染色体末端上的八个端粒基因的串联,发现端粒缩短期间表达的变化是不连续的,某些变化是衰老特异性而不是非分裂相关的。这些结果表明,天然端粒基因的表达可能受到局部异染色质结构改变的影响。

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