Faculty of Pharmacy, Drug Information Center, Minia University, Minia, 61519, Egypt.
Department of Biochemistry and Molecular Biology, Faculty of Pharmacy, Deraya University, Minia, 61111, Egypt.
Sci Rep. 2024 May 31;14(1):12566. doi: 10.1038/s41598-024-62740-6.
Testicular torsion carries the ominous prospect of inducing acute scrotal distress and the perilous consequence of testicular atrophy, necessitating immediate surgical intervention to reinstate vital testicular perfusion, notwithstanding the paradoxical detrimental impact of reperfusion. Although no drugs have secured approval for this urgent circumstance, antioxidants emerge as promising candidates. This study aspires to illustrate the influence of eprosartan, an AT1R antagonist, on testicular torsion in rats. Wistar albino rats were meticulously separated into five groups, (n = 6): sham group, eprosartan group, testicular torsion-detorsion (T/D) group, and two groups of T/D treated with two oral doses of eprosartan (30 or 60 mg/kg). Serum testosterone, sperm analysis and histopathological examination were done to evaluate spermatogenesis. Oxidative stress markers were assessed. Bax, BCL-2, SIRT1, Nrf2, HO-1 besides cleaved caspase-3 testicular contents were estimated using ELISA or qRT-PCR. As autophagy markers, SQSTM-1/p62, Beclin-1, mTOR and AMPK were investigated. Our findings highlight that eprosartan effectively improved serum testosterone levels, testicular weight, and sperm count/motility/viability, while mitigating histological irregularities and sperm abnormalities induced by T/D. This recovery in testicular function was underpinned by the activation of the cytoprotective SIRT1/Nrf2/HO-1 axis, which curtailed testicular oxidative stress, indicated by lowering the MDA content and increasing GSH content. In terms of apoptosis, eprosartan effectively countered apoptotic processes by decreasing cleaved caspase-3 content, suppressing Bax and stimulating Bcl-2 gene expression. Simultaneously, it reactivated impaired autophagy by increasing Beclin-1 expression, decreasing the expression of SQSTM-1/p62 and modulate the phosphorylation of AMPK and mTOR proteins. Eprosartan hold promise for managing testicular dysfunction arising from testicular torsion exerting antioxidant, pro-autophagic and anti-apoptotic effect via the activation of SIRT1/Nrf2/HO-1 as well as Beclin-1/AMPK/mTOR pathways.
睾丸扭转存在诱发急性阴囊疼痛和睾丸萎缩的险恶前景,需要立即进行手术干预以恢复重要的睾丸灌注,尽管再灌注存在矛盾的有害影响。尽管没有药物为此紧急情况获得批准,但抗氧化剂成为有前途的候选药物。本研究旨在说明 AT1R 拮抗剂依普罗沙坦对大鼠睾丸扭转的影响。Wistar 白化大鼠被精心分为五组,(n=6):假手术组、依普罗沙坦组、睾丸扭转-复位(T/D)组和两组用依普罗沙坦(30 或 60mg/kg)进行两次口服治疗的 T/D 组。进行血清睾酮、精子分析和组织病理学检查以评估精子发生。评估氧化应激标志物。使用 ELISA 或 qRT-PCR 估计睾丸内容物中的 Bax、BCL-2、SIRT1、Nrf2、HO-1 以及 cleaved caspase-3。作为自噬标志物,研究了 SQSTM-1/p62、Beclin-1、mTOR 和 AMPK。我们的研究结果表明,依普罗沙坦可有效提高血清睾酮水平、睾丸重量和精子计数/活力/活力,同时减轻 T/D 引起的组织学异常和精子异常。这种睾丸功能的恢复是由保护性 SIRT1/Nrf2/HO-1 轴的激活来支撑的,该轴通过降低 MDA 含量和增加 GSH 含量来减少睾丸氧化应激。就细胞凋亡而言,依普罗沙坦通过降低 cleaved caspase-3 含量、抑制 Bax 和刺激 Bcl-2 基因表达来有效对抗细胞凋亡过程。同时,它通过增加 Beclin-1 表达、降低 SQSTM-1/p62 的表达以及调节 AMPK 和 mTOR 蛋白的磷酸化来重新激活受损的自噬。依普罗沙坦有望通过激活 SIRT1/Nrf2/HO-1 以及 Beclin-1/AMPK/mTOR 途径发挥抗氧化、促进自噬和抗细胞凋亡作用,从而治疗由睾丸扭转引起的睾丸功能障碍。
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