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人类精子发生过程中相对端粒长度谱随年龄的变化。

Age-dependence of relative telomere length profiles during spermatogenesis in man.

机构信息

Laboratory of Reproductive Biology, Scientific Unit, Horsens Hospital, Denmark.

出版信息

Maturitas. 2013 Aug;75(4):380-5. doi: 10.1016/j.maturitas.2013.05.001. Epub 2013 Jun 10.

DOI:10.1016/j.maturitas.2013.05.001
PMID:23764353
Abstract

Telomeres, the protective structures at the outmost ends of chromosomes, shorten in all somatic cells with each cell-division and by cumulative oxidative damage. To counteract that these shortened telomeres are passed on to offspring, the telomeres are elongated by the enzyme, telomerase, during human spermatogenesis. A few groups have tried to elucidate this process by measuring telomerase activity in the various cell-types during spermatogenesis, but until now, no one has ever measured telomere length (TL) during these different stages in humans. Some groups have measured TL in spermatozoa and surprisingly found that telomeres of older men are longer, than those from younger men. To elucidate this phenomenon we investigated if the distribution of TL over the various precursor germ cells in old males differed from young males, perhaps indicating a more ubiquitous telomere elongation in testes from older men. We therefore obtained testicular biopsies from 6 older and 6 younger men undergoing vasectomy. The cells were suspended as single cells and smeared onto slides, followed by characterization of cell stages by phase contrast microscopy. Mean TL in individual cells was subsequently measured by telomere QFISH. Our data revealed no difference in the TL profile during spermatogenesis between younger and older men. All men had a similar profile which strongly resembled the telomerase expression profile found by others. This indicates that the longer telomeres in older men are not caused by a wider window of telomere elongation, stretching over more cell-types of spermatogenesis.

摘要

端粒是染色体末端的保护结构,在所有体细胞中,随着细胞分裂和累积的氧化损伤,端粒会逐渐缩短。为了防止这些缩短的端粒传递给后代,端粒酶在人类精子发生过程中会延长端粒。一些研究小组试图通过测量精子发生过程中各种细胞类型中端粒酶的活性来阐明这个过程,但到目前为止,还没有人在人类的这些不同阶段测量过端粒长度(TL)。一些研究小组测量了精子中的 TL,令人惊讶的是,他们发现年长男性的端粒比年轻男性的端粒更长。为了阐明这一现象,我们研究了老年男性睾丸中各种前体细胞中端粒长度的分布是否与年轻男性不同,也许这表明老年男性睾丸中端粒的延长更为普遍。因此,我们从 6 名接受输精管切除术的老年男性和 6 名年轻男性中获得了睾丸活检。将细胞悬浮为单细胞并涂抹在载玻片上,然后通过相差显微镜对细胞阶段进行特征描述。随后通过端粒 QFISH 测量单个细胞中的平均 TL。我们的数据显示,年轻男性和老年男性之间的精子发生中端粒长度的分布没有差异。所有男性的 TL 分布模式都相似,与其他人发现的端粒酶表达模式非常相似。这表明,年长男性的端粒较长不是由于更广泛的端粒延长窗口,延伸到更多的精子发生细胞类型。

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