Sirtuin 1-mediated autophagy regulates testosterone synthesis in Leydig cells of piglets

IF 2.4 2区 农林科学 Q3 REPRODUCTIVE BIOLOGY Theriogenology Pub Date : 2024-09-14 DOI:10.1016/j.theriogenology.2024.09.010
Yanyan Zhang , Lingyun Yu , Yijing He , Chengyin Liu , Mahmoud M. Abouelfetouh , Shiqiang Ju , Zhenlei Zhou , Qiao Li
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Abstract

Testosterone is secreted by Leydig cells (LCs), which play an important physiological role in preserving male secondary sex characteristics, protecting male reproductive function, and establishing the blood-testis barrier. Studies have shown that autophagy is particularly active in LCs; however, its involvement in testosterone synthesis in porcine LCs has not been fully explored. Therefore, this experiment aimed to investigate the influence of autophagy on testosterone secretion in porcine LCs and its potential regulatory mechanism. Our results demonstrated that both testicular autophagy and serum testosterone levels increased in piglets during postnatal development from 4 to 18 weeks. In addition, autophagy was found to degrade the Na+/H+ exchange regulatory factor 2 (NHERF2), leading to the up-regulation of scavenger receptor class B type 1 (SRB1). This process resulted in increased cholesterol intake and enhanced testosterone production. The observable level of sirtuin 1 (SIRT1) was directly proportional to the level of autophagy. In vitro investigations have shown that SIRT1 can affect the level of autophagy, cholesterol uptake as well as testosterone release. In conclusion, testosterone synthesis during pig development is regulated by SIRT1. SIRT1 mediates the degradation of NHERF2 through autophagy, thereby weakening its negative regulatory effect on the high-density lipoprotein receptor SRB1 in Leydig cells. This process increases cholesterol uptake and enhances testosterone synthesis.

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Sirtuin 1 介导的自噬调节仔猪睾丸激素的合成
睾酮由莱德细胞(Leydig cells,LCs)分泌,在保持男性第二性征、保护男性生殖功能和建立血液-睾丸屏障方面发挥着重要的生理作用。研究表明,自噬在LCs中特别活跃;然而,自噬在猪LCs中参与睾酮合成的情况尚未得到充分探讨。因此,本实验旨在研究自噬对猪睾丸细胞睾酮分泌的影响及其潜在的调控机制。我们的结果表明,仔猪在出生后 4 至 18 周的发育过程中,睾丸自噬和血清睾酮水平均有所上升。此外,我们还发现自噬可降解Na+/H+交换调节因子2(NHERF2),从而导致清道夫受体B类1(SRB1)的上调。这一过程导致胆固醇摄入量增加,睾酮分泌增强。sirtuin 1(SIRT1)的可观察水平与自噬水平成正比。体外研究表明,SIRT1 可影响自噬水平、胆固醇摄取量和睾酮释放量。总之,猪发育过程中睾酮的合成受 SIRT1 的调控。SIRT1 通过自噬作用介导 NHERF2 的降解,从而削弱其对雷迪格细胞中高密度脂蛋白受体 SRB1 的负面调节作用。这一过程增加了胆固醇的吸收,并促进了睾酮的合成。
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来源期刊
Theriogenology
Theriogenology 农林科学-生殖生物学
CiteScore
5.50
自引率
14.30%
发文量
387
审稿时长
72 days
期刊介绍: Theriogenology provides an international forum for researchers, clinicians, and industry professionals in animal reproductive biology. This acclaimed journal publishes articles on a wide range of topics in reproductive and developmental biology, of domestic mammal, avian, and aquatic species as well as wild species which are the object of veterinary care in research or conservation programs.
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