The SPARC-related modular calcium binding 1 ( Smoc1 ) regulated by androgen is required for mouse gubernaculum development and testicular descent.

Asian journal of andrology Pub Date : 2025-01-01 Epub Date: 2024-08-09 DOI:10.4103/aja202449
Zhi-Yi Zhao, Yong Siow, Ling-Yun Liu, Xian Li, Hong-Liang Wang, Zhen-Min Lei
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Abstract

Abstract: Testicular descent occurs in two consecutive stages: the transabdominal stage and the inguinoscrotal stage. Androgens play a crucial role in the second stage by influencing the development of the gubernaculum, a structure that pulls the testis into the scrotum. However, the mechanisms of androgen actions underlying many of the processes associated with gubernaculum development have not been fully elucidated. To identify the androgen-regulated genes, we conducted large-scale gene expression analyses on the gubernaculum harvested from luteinizing hormone/choriogonadotropin receptor knockout ( Lhcgr KO) mice, an animal model of inguinoscrotal testis maldescent resulting from androgen deficiency. We found that the expression of secreted protein acidic and rich in cysteine (SPARC)-related modular calcium binding 1 ( Smoc1 ) was the most severely suppressed at both the transcript and protein levels, while its expression was the most dramatically induced by testosterone administration in the gubernacula of Lhcgr KO mice. The upregulation of Smoc1 expression by testosterone was curtailed by the addition of an androgen receptor antagonist, flutamide. In addition, in vitro studies demonstrated that SMOC1 modestly but significantly promoted the proliferation of gubernacular cells. In the cultures of myogenic differentiation medium, both testosterone and SMOC1 enhanced the expression of myogenic regulatory factors such as paired box 7 ( Pax7 ) and myogenic factor 5 ( Myf5 ). After short-interfering RNA-mediated knocking down of Smoc1 , the expression of Pax7 and Myf5 diminished, and testosterone alone did not recover, but additional SMOC1 did. These observations indicate that SMOC1 is pivotal in mediating androgen action to regulate gubernaculum development during inguinoscrotal testicular descent.

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受雄激素调控的SPARC相关模块化钙结合1(Smoc1)是小鼠睾丸发育和睾丸下降所必需的。
摘要:睾丸下降分为两个连续的阶段:经腹阶段和阴囊内阶段。雄激素在第二阶段中起着至关重要的作用,它影响着gubernaculum的发育,gubernaculum是一种将睾丸拉入阴囊的结构。然而,与睾丸阴囊发育相关的许多过程的雄激素作用机制尚未完全阐明。为了确定受雄激素调控的基因,我们对从黄体生成素/绒毛促性腺激素受体敲除(Lhcgr KO)小鼠身上采集的gubernaculum进行了大规模基因表达分析。我们发现,酸性富含半胱氨酸的分泌蛋白(SPARC)相关模块化钙结合1(Smoc1)的表达在转录本和蛋白水平上都受到了最严重的抑制,而在Lhcgr KO小鼠的睾丸中,睾酮对其表达的诱导作用最为显著。加入雄激素受体拮抗剂氟他胺后,睾酮对Smoc1表达的上调作用被抑制。此外,体外研究表明,SMOC1 能适度但显著地促进脐带细胞的增殖。在成肌分化培养基中,睾酮和 SMOC1 都能增强成肌调节因子的表达,如配对盒 7(Pax7)和成肌因子 5(Myf5)。在短干扰 RNA 介导的 Smoc1 敲除后,Pax7 和 Myf5 的表达减弱,单用睾酮不能恢复,但添加 SMOC1 则能恢复。这些观察结果表明,在腹股沟睾丸下降过程中,SMOC1在介导雄激素作用以调节鞘膜发育方面起着关键作用。
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