壮腰健腰丸可改善睾酮诱导的大鼠良性肝后增生。

Zheng Jingrui, Chen Weijian, Y E Binbin, M O Ziyao, D U Qunqun, Qin Renan, Nie Ke
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引用次数: 0

摘要

目的确定壮阳健脾丸(ZYJSP)对良性前列腺增生症(BPH)的治疗作用,并探讨其潜在机制:方法:将48只雄性Sprague-Dawley大鼠随机分为6组:对照组、良性前列腺增生模型组、非那雄胺处理组、ZYJSP低、中、高剂量组。除对照组外,其余 40 只大鼠均被阉割,并连续 28 天注射丙酸睾酮(TP)诱导良性前列腺增生。同时灌胃相应的药物。测定前列腺湿重、前列腺指数(PI)和前列腺组织病理学变化,作为研究 ZYJSP 对良性前列腺增生症疗效的依据。测定血清性激素水平、氧化应激标志物、炎症标志物、肾功能标志物、生长因子和前列腺中 Cyclin D1 的表达,以确定 ZYJSP 对良性前列腺增生症的治疗机制:结果:服用 ZYJSP 能明显减轻 TP 治疗的阉割大鼠的前列腺湿重和 PI,并改善前列腺的组织学变化。TP明显增加了血清中肌酐、血尿素氮和生长因子的水平,也增加了前列腺中细胞周期蛋白D1的表达。ZYJSP 能显著降低这些指标中的大部分。ZYJSP 能明显恢复 TP 引起的睾酮、雌二醇和双氢睾酮的失调。此外,ZYJSP 还能缓解 TP 引起的前列腺损伤,并通过降低白细胞介素-6、白细胞介素-8 和丙二醛水平以及提高血清中超氧化物歧化酶的活性,表现出抗炎和抗氧化活性:这些研究结果表明,ZYJSP能有效改善阉割大鼠由TP诱导的良性前列腺增生症,其潜在机制可能与调节性激素平衡、减少氧化应激和抑制炎症反应有关。
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Zhuangyao Jianshen pill ameliorates testosterone-induced benign postatic hyperplasia in rats.

Objective: To determine the therapeutic effects of the Zhuangyao Jianshen pill (, ZYJSP) against benign prostatic hyperplasia (BPH) and investigate the underlying mechanism.

Methods: Forty-eight male Sprague-Dawley rats were randomly divided into six groups: Control group, BPH model group, finasteride-treated group, ZYJSP low, medium and high dose groups. Except for the control group, 40 rats were castrated and injected with testosterone propionate (TP) for 28 consecutive day to induce BPH. Meanwhile, the corresponding drugs were administered by gavage. The prostate wet weight, prostate index (PI), and the histopathological changes in the prostate were measured as the basis for examining the efficacy of ZYJSP against BPH. Levels of the serum sex hormones, oxidative stress markers, inflammatory markers, renal function markers, growth factors, and Cyclin D1 expression in prostate were measured to characterize the therapeutic mechanism of ZYJSP against BPH.

Results: ZYJSP administration significantly reduced prostate wet weight and PI and ameliorated histological changes of the prostate in TP-treated castrated rats. TP markedly increased the levels of creatinine, blood urea nitrogen and growth factors in the serum as well as the expression of the Cyclin D1 in the prostate. Most of these markers were significantly decreased by ZYJSP. ZYJSP significantly restored the dysregulation of testosterone, estradiol, and dihydrotestosterone caused by TP. Furthermore, ZYJSP relieved TP-induced prostate injury and exhibited both anti-inflammatory and anti-oxidant activity by decreasing interleukin-6, interleukin-8, and malondialdehyde levels and increasing the activity of superoxide dismutase in the serum.

Conclusion: These findings indicate that ZYJSP can effectively ameliorate BPH induced by TP in castrated rats, and the underlying mechanism might be related to regulating sex hormone balance, reducing oxidative stress, and inhibiting the inflammatory response.

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