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Expression dynamics of self-renewal factors for spermatogonial stem cells in the mouse testis

机译:小鼠睾丸精原干细胞自我更新因子的表达动态

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摘要

Glial cell line-derived neurotrophic factor (GDNF) and fibroblast growth factor 2 (FGF2) are bona fide self-renewal factors for spermatogonial stem cells (SSCs). Although GDNF is indispensable for the maintenance of SSCs, the role of FGF2 in the testis remains to be elucidated. To clarify this, the expression dynamics and regulatory mechanisms of Fgf2 and Gdnf in the mouse testes were analyzed. It is well known that Sertoli cells express Gdnf, and its receptor is expressed in a subset of undifferentiated spermatogonia, including SSCs. However, we found that Fgf2 was mainly expressed in the germ cells and its receptors were expressed not only in the cultured spermatogonial cell line, but also in testicular somatic cells. Aging, hypophysectomy, retinoic acid treatment, and testicular injury induced distinct Fgf2 and Gdnf expression dynamics, suggesting a difference in the expression mechanism of Fgf2 and Gdnf in the testis. Such differences might cause a dynamic fluctuation of Gdnf/Fgf2 ratio depending on the intrinsic/extrinsic cues. Considering that FGF2-cultured spermatogonia exhibit more differentiated phenotype than those cultured with GDNF, FGF2 might play a role distinct from that of GDNF in the testis, despite the fact that both factors are self-renewal factor for SSC in vitro.
机译:胶质细胞源性神经营养因子(GDNF)和成纤维细胞生长因子2(FGF2)是精原干细胞(SSCs)的真正自我更新因子。尽管GDNF对于维持SSC是必不可少的,但FGF2在睾丸中的作用仍有待阐明。为了阐明这一点,分析了Fgf2和Gdnf在小鼠睾丸中的表达动力学和调控机制。众所周知,支持细胞表达Gdnf,其受体在未分化的精原细胞的一个子集(包括SSC)中表达。但是,我们发现Fgf2主要在生殖细胞中表达,其受体不仅在培养的精原细胞系中表达,而且在睾丸体细胞中表达。衰老,垂体切除术,维甲酸治疗和睾丸损伤诱导了不同的Fgf2和Gdnf表达动力学,表明Fgf2和Gdnf在睾丸中的表达机制有所不同。这种差异可能会导致Gdnf / Fgf2比的动态波动,具体取决于内部/外部线索。考虑到用FGF2培养的精原细胞比用GDNF培养的精原细胞表现出更高的分化表型,尽管这两个因素都是体外SSC的自我更新因子,但FGF2可能在睾丸中的作用不同于GDNF。

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