Testis development is dependent on the key sex-determining factors SRY and SOX9, which activate the essential ligand FGF9. Although FGF9 plays a central role in testis development, it is unable to induce testis formation on its own. However, other growth factors, including activins and TGFβs, also present testis during testis formation. In this study, we investigated the potential of FGF9 combined with activin and TGFβ to induce testis development in cultured XX gonads. Our data demonstrated differing individual and combined abilities of FGF9, activin and TGFβ to promote supporting cell proliferation, Sertoli cell development and male germ line differentiation in cultured XX gonads. FGF9 promoted proliferation of supporting cells in XX foetal gonads at rates similar to those observed in vivo during testis cord formation in XY gonads but was insufficient to initiate testis development. However, when FGF9, activin and TGFβ were combined, aspects of testicular development were induced, including the expression of Sox9, morphological reorganisation of the gonad and deposition of laminin around germ cells. Enhancing β-catenin activity diminished the testis-promoting activities of the combined growth factors. The male promoting activity of FGF9 and the combined growth factors directly or indirectly extended to the germ line, in which a mixed phenotype was observed. FGF9 and the combined growth factors promoted male germ line development, including mitotic arrest, but expression of pluripotency genes was maintained, rather than being repressed. Together, our data provide evidence that combined signalling by FGF9, activin and TGFβ can induce testicular characteristics in XX gonads.

译文

睾丸发育取决于关键的性别决定因素SRY和SOX9,它们激活了必需配体fgf9。尽管FGF9在睾丸发育中起着核心作用,但它无法自行诱导睾丸形成。然而,其他生长因子,包括激活素和转化生长因子 β,在睾丸形成过程中也存在睾丸。在这项研究中,我们研究了FGF9与激活素和tgf β 结合在培养的XX性腺中诱导睾丸发育的潜力。我们的数据表明,FGF9,激活素和tgf β 在促进培养的XX性腺中支持细胞增殖,支持细胞发育和雄性种系分化方面具有不同的个体和综合能力。FGF9促进XX胎儿性腺中支持细胞的增殖,其速率与XY性腺中睾丸索形成过程中体内观察到的速率相似,但不足以启动睾丸发育。然而,当FGF9,激活素和tgf β 结合时,会诱导睾丸发育的各个方面,包括Sox9的表达,性腺的形态重组和层粘连蛋白在生殖细胞周围的沉积。增强 β-catenin活性会降低联合生长因子的睾丸促进活性。FGF9和组合生长因子的雄性促进活性直接或间接扩展到种系,其中观察到混合表型。FGF9和组合的生长因子促进了雄性种系的发育,包括有丝分裂停滞,但多能性基因的表达得以维持,而不是被抑制。总之,我们的数据提供了证据,表明FGF9,激活素和tgf β 的联合信号可以诱导XX性腺的睾丸特征。

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