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成年莱迪希干细胞的鉴定、增殖和分化。

Identification, proliferation, and differentiation of adult Leydig stem cells.

机构信息

Department of Biochemistry and Molecular Biology, Johns Hopkins Bloomberg School of Public Health, Baltimore, Maryland 21205, USA.

出版信息

Endocrinology. 2012 Oct;153(10):5002-10. doi: 10.1210/en.2012-1417. Epub 2012 Aug 3.

Abstract

Leydig cells, the testosterone-producing cells of the adult testis, rarely turn over. However, their elimination with ethane dimethanesulfonate (EDS) is followed by the appearance of new, fully functional adult Leydig cells. The cells that give rise to the new Leydig cells have not been well characterized, and little is known about the mechanism by which they are regulated. We isolated cells expressing platelet-derived growth factor receptor-α, but not 3β-hydroxysteroid dehydrogenase (3β-HSD(neg)) from the testes of EDS-treated adult rats. Depending on conditions, these cells proliferated indefinitely or differentiated and produced testosterone. To localize these cells and to determine the effect of the testicular environment on their function, the seminiferous tubules and testicular interstitium were physically separated and cultured. During the first 72 h in culture, 3β-HSD(neg) cells on the tubule surfaces underwent divisions. Some of these cells later expressed 3β-HSD and produced testosterone. Removal of the newly formed 3β-HSD(pos) cells from the tubule surfaces with EDS, followed by further culture of the stripped tubules, resulted in the reappearance of testosterone-producing cells. These results, taken together, suggest that the precursors for newly formed Leydig cells are stem cells, with many if not all situated on the surfaces of the seminiferous tubules. Although normally quiescent, the stem cells are capable of self-renewal and differentiation. The development of the tubule culture system should provide a valuable in vitro approach to assess the role(s) of niche components on the function of adult Leydig stem cells despite their residing in a complex mammalian tissue.

摘要

睾丸间质细胞是成年睾丸中产生睾酮的细胞,它们很少有更新。然而,用乙烷二甲基亚砜(EDS)消除它们后,会出现新的、具有完全功能的成年睾丸间质细胞。产生新的睾丸间质细胞的细胞尚未得到很好的描述,并且对于调节这些细胞的机制知之甚少。我们从 EDS 处理的成年大鼠的睾丸中分离出表达血小板衍生生长因子受体-α但不表达 3β-羟类固醇脱氢酶(3β-HSD(neg))的细胞。根据条件的不同,这些细胞可以无限增殖或分化并产生睾酮。为了定位这些细胞并确定睾丸环境对其功能的影响,我们将生精小管和睾丸间质物理分离并进行培养。在培养的前 72 小时内,小管表面的 3β-HSD(neg)细胞发生分裂。其中一些细胞后来表达 3β-HSD 并产生睾酮。用 EDS 从小管表面去除新形成的 3β-HSD(pos)细胞,然后进一步培养剥离的小管,导致产生睾酮的细胞再次出现。这些结果表明,新形成的睾丸间质细胞的前体细胞是干细胞,其中许多(如果不是全部)位于生精小管的表面。尽管通常处于静止状态,但干细胞具有自我更新和分化的能力。尽管这些干细胞位于复杂的哺乳动物组织中,但小管培养系统的发展应该为评估小生境成分对成年睾丸间质干细胞功能的作用提供有价值的体外方法。

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