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Effects of Osteocalcin on Synthesis of Testosterone and INSL3 during Adult Leydig Cell Differentiation

机译:骨钙素对成年Leydig细胞分化过程中睾丸激素和INSL3合成的影响

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摘要

Proliferation and differentiation of adult Leydig cells are mainly completed in puberty. In many studies, apart from normal postnatal development process, it is widely indicated that, through administrating EDS, Leydig cell population is eliminated and regenerated. It is believed that osteocalcin released from osteoblasts, which is responsible for modulating bone metabolism, induces testosterone production in Leydig cells, independent of the HPG axis. In addition, INSL3 produced by Leydig cells, such as testosterone, plays a critical role in bone metabolism and is known to reflect the development process and functional capacities of Leydig cells. This study is aimed at investigating OC-mediated testosterone regulation and INSL3 synthesis during differentiation of adult Leydig cells that are independent of LH. For this purpose, male rats were divided into 2 groups: prepubertal normal rats and adult EDS-injected rats. Each group was divided into 4 subgroups in which GnRH antagonist or OC was applied. After adult Leydig cells completed their development, testicular tissue samples obtained from the sacrificed rats were examined by light-electron microscopic, immunohistochemical, and biochemical methods. Slight upregulation in 3βHSD, INSL3, and GPRC6A expressions along with the increase in serum testosterone levels was observed in groups treated with osteocalcin against GnRH antagonist. In addition, biochemical and microscopic findings in osteocalcin treated groups were similar to those in control groups. While there was no significant difference in the number of Leydig cells reported, the presence of a significant upregulation in INSL3 and GPRC6A expressions and the increase in serum testosterone and ucOC levels were observed. After evaluation of findings altogether, it is put forward that, for the first time in this study, although osteocalcin treatment made no significant difference in the number of Leydig cells, it increased the level of testosterone through improving the function of existing adult Leydig cells during normal postnatal development process and post-EDS regeneration. This positive correlation between osteocalcin-testosterone and osteocalcin-INSL3 is concluded to be independent of LH at in vivo conditions.
机译:成年Leydig细胞的增殖和分化主要在青春期完成。在许多研究中,除正常的产后发育过程外,广泛表明,通过施用EDS,Leydig细胞群得以消除和再生。据信,从成骨细胞释放的骨钙素负责调节骨代谢,可诱导Leydig细胞中的睾丸激素产生,而与HPG轴无关。另外,由睾丸间质细胞(Leydig cell)产生的INSL3(例如睾丸激素)在骨代谢中起着关键作用,并且已知其反映了睾丸间质细胞的发育过程和功能能力。这项研究旨在调查成年的Leydig细胞独立于LH分化过程中OC介导的睾丸激素调节和INSL3合成。为此,将雄性大鼠分为两组:青春期前正常大鼠和成年EDS注射大鼠。每组分为4个亚组,分别应用GnRH拮抗剂或OC。成年Leydig细胞完成发育后,通过光电子显微镜,免疫组织化学和生化方法检查从处死的大鼠获得的睾丸组织样品。在用骨钙蛋白抗GnRH拮抗剂治疗的组中观察到3βHSD,INSL3和GPRC6A表达略有上调,同时血清睾丸激素水平升高。此外,骨钙素治疗组的生化和显微镜检查结果与对照组相似。尽管报告的Leydig细胞数量没有显着差异,但观察到INSL3和GPRC6A表达明显上调,血清睾丸激素和ucOC水平增加。总体评估结果后,提出本研究中首次,尽管骨钙素治疗对Leydig细胞的数量没有显着影响,但它通过改善成年Leydig细胞的功能提高了睾丸激素的水平。正常的产后发育过程和EDS后的再生。结论:在体内条件下,骨钙素-睾丸激素和骨钙素-INSL3之间的这种正相关独立于LH。

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