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首页> 外文期刊>Reproduction: The official journal of the Society for the Study of Fertility >Elucidating human male germ cell development by studying germ cell cancer
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Elucidating human male germ cell development by studying germ cell cancer

机译:通过研究生殖细胞癌阐明人类男性生殖细胞发育

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摘要

Human germ cell development is regulated in a spatio-temporal manner by complex regulatory networks. Here, we summarize results obtained in germ cell tumors and respective cell lines and try to pinpoint similarities to normal germ cell development. This comparison allows speculating about the critical and error-prone mechanisms, which when disturbed, lead to the development of germ cell tumors. Short after specification, primordial germ cells express markers of pluripotency, which, in humans, persists up to the stage of fetal/infantile spermatogonia. Aside from the rare spermatocytic tumors, virtually all seminomas and embryonal carcinomas express markers of pluripotency and show signs of pluripotency or totipotency. Therefore, it appears that proper handling of the pluripotency program appears to be the most critical step in germ cell development in terms of tumor biology. Furthermore, data from mice reveal that germline cells display an epigenetic signature, which is highly similar to pluripotent cells. This signature (poised histone code, DNA hypomethylation) is required for the rapid induction of toti- and pluripotency upon fertilization. We propose that adult spermatogonial cells, when exposed to endocrine disruptors or epigenetic active substances, are prone to reinitiate the pluripotency program, giving rise to a germ cell tumor. The fact that pluripotent cells can be derived from adult murine and human testicular cells further corroborates this idea.
机译:人类生殖细胞的发育通过复杂的调控网络以时空方式调控。在这里,我们总结了在生殖细胞肿瘤和各个细胞系中获得的结果,并试图指出与正常生殖细胞发育的相似性。这种比较允许推测关键的和容易出错的机制,这些机制在受到干扰时会导致生殖细胞肿瘤的发展。规范后不久,原始生殖细胞表达多能性标志物,在人类中,这种多能性标志物一直持续到胎儿/婴儿精原细胞的阶段。除了罕见的精子细胞肿瘤,几乎所有的精原细胞瘤和胚胎癌都表达多能性标志物,并显示出多能性或全能性的迹象。因此,就肿瘤生物学而言,似乎对多能性程序的正确处理似乎是生殖细胞发育中最关键的一步。此外,来自小鼠的数据表明种系细胞表现出表观遗传学特征,与多能细胞高度相似。此标记(平衡的组蛋白代码,DNA低甲基化)是受精后快速诱导全能和全能所必需的。我们建议,成年的精原细胞暴露于内分泌干扰物或表观遗传活性物质时,很容易重新启动多能性程序,从而引起生殖细胞肿瘤。多能细胞可以来自成年鼠和人睾丸细胞的事实进一步证实了这一想法。

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