Apoptosis is an important regulatory event in testicular homeostasis and optimization of sperm production. Sertoli cells (SCs) form the blood-testis barrier creating a special microenvironment where germ cells develop and are under strict hormonal control. Estrogens and androgens are known to play critical roles in SCs functioning, improving their in vitro survival by preventing apoptotic progression. Herein, we studied the influence of 17β-estradiol (E2) and 5α-dihydrotestosterone (DHT) on the apoptotic signaling pathways of immature rat cultured SCs. For that we chose key points of the apoptotic pathway that interact with the mitochondria and evaluated the mRNA expression and/or protein levels of several apoptotic markers such as p53, the anti-apoptotic protein Bcl2, the pro-apoptotic Bcl2 family member Bax, the apoptosis-inducing factor (AIF) and caspase-3 and 9. Caspase-3 activity and DNA fragmentation were also evaluated as endpoint markers of apoptosis. E2 and DHT down-regulated the mRNA transcript levels of p53, Bax, caspase-9 and caspase-3. The protein levels of AIF were reduced after DHT treatment while E2-treated cells presented decreased levels of cleaved caspase-9 protein. Moreover, Bax/Bcl2 ratio was significantly decreased in E2-treated cells. The apoptotic endpoints caspase-3 activity and DNA fragmentation presented significant decreased levels after hormonal treatment. Taken together, these results show that E2 and DHT act as apoptotic signaling modulators in in vitro immature rat SCs suggesting that androgens and estrogens may be capable of modulating independent pathways of the apoptotic event by regulating different pro-apoptotic factors.

译文

细胞凋亡是睾丸稳态和精子生成优化的重要调节事件。支持细胞 (SCs) 形成血液-睾丸屏障,创造了一个特殊的微环境,生殖细胞发育并受到严格的激素控制。已知雌激素和雄激素在SCs功能中起关键作用,通过防止凋亡进程来改善其体外存活。本文研究了17β-雌二醇 (E2) 和5α-二氢睾酮 (DHT) 对未成熟大鼠SCs凋亡信号通路的影响。为此,我们选择了与线粒体相互作用的凋亡途径的关键点,并评估了几种凋亡标志物的mRNA表达和/或蛋白水平,例如p53,抗凋亡蛋白Bcl2,促凋亡Bcl2家族成员Bax,凋亡诱导因子 (AIF) 与caspase-3和9。Caspase-3活性和DNA片段也被评估为凋亡的终点标记。E2和DHT下调了p53,Bax,caspase-9和caspase-3的mRNA转录水平。DHT处理后AIF的蛋白质水平降低,而E2-treated细胞的裂解caspase-9蛋白水平降低。此外,E2-treated细胞中的Bax/Bcl2比率显着降低。激素治疗后,凋亡终点caspase-3活性和DNA片段化水平显着降低。总之,这些结果表明E2和DHT在体外未成熟大鼠SCs中充当凋亡信号调节剂,这表明雄激素和雌激素可能能够通过调节不同的促凋亡因子来调节凋亡事件的独立途径。

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