左归丸、右桂丸对小鼠围绝经期综合征细胞凋亡的调节作用。

Wang Tianqi, L I Zining, Chen Ting, Chen Rui, Jin Ya, Oduro Patrick Kwabena, Zhang Han, Wang Yi
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引用次数: 0

摘要

目的:观察、解剖、了解左归丸(ZGP)与优归丸(YGP)治疗4-乙烯基二氧化环己烯(4-VCD)所致围绝经期综合征(PMS)的分子机制及联合作用。方法:采用4- vcd诱导的经前综合征小鼠模型,测定ZGP、YGP、ZGP + YGP、戊酸雌二醇(EV)、更年安(ggnan,更年安,GNA)治疗后小鼠子宫和卵巢指数,测定血清性甾体激素水平。通过组织病理学检查、成分-靶点网络预测、western blotting和实时定量聚合酶链反应(RT-qPCR)分析,确定ZYP和YGP可能的药理作用和分子机制。结果:ZGP和YGP治疗可明显改善动情周期,防止子宫病理损害。此外,改变性激素,包括AMH、E2、FSH、LH、P和T,在ZGP和YGP治疗后恢复到正常水平。成分-靶点网络分析表明,ZGP和YGP两方共有的5种成分调节了PMS共有的53个靶点。通路富集分析进一步预测ZGY和YGP可能调控PMS期间细胞凋亡等重要通路。体内研究表明,ZGP和YGP通过降低Caspase-3和Bcl-2相关X (Bax)水平,增加b细胞淋巴瘤-2 (Bcl-2)/Bax和Bcl-2水平,抑制PMS调节细胞凋亡。重要的是,与ZGP或YGP单独治疗相比,ZGP + YGP治疗的调节效果有所或显著更好。结论:ZGP和YGP是一种新型的抗经前症候群药物,其作用包括恢复激素水平、保护子宫和调节细胞凋亡。
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Zuogui and Yougui pills improve perimenopausal syndrome regulation of apoptosis in mice.

Objective: To examine, dissect, and understand the molecular mechanisms and combinatorial effects of Zuogui (, ZGP) and Yougui pills (, YGP) in 4-vinyl cyclohexene diepoxide (4-VCD)-induced Perimenopausal syndrome (PMS).

Methods: Using the 4-VCD-induced PMS mouse model, uterine and ovary index were measured, and serum sex steroidal hormone levels were evaluated after treatment with ZGP, YGP, ZGP + YGP, estradiol valerate (EV), and Gengnian An (gengnianan, GNA). Histopathological examinations, ingredient-target network predictions, western blotting, and real-time quantitative polymerase chain reaction (RT-qPCR) analyses were performed to ascertain the possible pharmacological effects and molecular mechanisms of ZYP and YGP.

Results: Treatment with ZGP and YGP remarkably improves estrous cyclicity and prevents pathological damage to the uterus. Also, altered sex hormones, including AMH, E2, FSH, LH, P, and T, were restored to normal levels after ZGP and YGP administration. Ingredient-target network analysis showed that the 5 ingredients common to the ZGP and YGP formula modulate 53 targets shared with PMS. Pathway-enrichment analysis further predicted that ZGY and YGP likely regulate of apoptosis and other essential pathways during PMS. In-vivo studies showed that ZGP and YGP suppress PMS modulating apoptosis through decreasing Caspase-3 and Bcl-2-associated X (Bax) levels and increasing B-cell lymphoma-2 (Bcl-2)/Bax and Bcl-2 levels. Importantly, ZGP + YGP treatment modulation effects were somewhat or significantly better compared to ZGP or YGP alone treatment.

Conclusion: ZGP and YGP represent novel anti-PMS agents whose effects involve restoring altered hormonal levels, protecting the uterus, and regulating apoptosis.

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