Synergistic action of carvedilol and clomiphene in mitigating the behavioral phenotypes of letrozole-model of PCOS rats by modulating the NRF2/NFKB pathway.

O. Akintoye, A. Ajibare, Isaac A. Oriyomi, B. Olofinbiyi, Yusuf Grace Oyiza, Afuye Damilola Christanah, T. Babalola, Faturoti Oluwadamilola Esther, Oludipe Seun, V. B. Owoyele
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引用次数: 1

Abstract

INTRODUCTION Psychiatric and cognitive impairment has been observed in premenopausal women with a hormonal disorder called polycystic ovary syndrome (PCOS). This study aimed to explore the possibility of combining pharmacological agents: Carvedilol and Clomiphene citrate, with antiestrogenic, antioxidant and anti-inflammatory properties in letrozole-induced PCOS rats. METHODS PCOS was induced in rats by the administration of letrozole (1 mg/kg) daily for 21 days. They were subsequently divided into four groups, each receiving either the vehicle or Clomiphene citrate (1 mg/kg) or Carvedilol or a combination of Clomiphene citrate and Carvedilol, respectively from days 22-36. Neurobehavioral studies were conducted on day 35 (Elevated plus maze and Y maze) and day 36 (Novel object recognition). The serum levels of the antioxidants Superoxide dismutase, Catalase, Interleukin 1B (IL-1B), and the gene expression of nuclear factor-erythroid factor 2-related factor 2 (Nrf2), Nuclear Factor k-Beta (NFKB), and acetylcholine esterase in the frontal brain homogenate was determined. RESULT Both Carvedilol and the combination therapy reversed the anxiety-like behavior, while Clomiphene citrate and the combination therapy ameliorated the spatial and non-spatial memory impairment observed in PCOS rats. Carvedilol, Clomiphene citrate, and the combination therapy increased the serum concentration of SOD and Catalase and decreased the serum concentration of IL-1B. The combination therapy up-regulated the NRF-2, NFKB, and acetylcholine esterase gene expression. CONCLUSION Study showed that the combination of carvedilol and clomiphene citrate has anxiolytic potential and improved cognitive functions in PCOS rats. This might have been achieved by carvedilol and clomiphene citrate's ability to modulate the cholinergic system and the Nrf2 pathway while downregulating the NFκB signaling pathway.
卡维地洛和克罗米芬通过调节NRF2/NFKB通路对来曲唑模型PCOS大鼠行为表型的协同作用
精神和认知障碍已被观察到绝经前妇女的荷尔蒙失调称为多囊卵巢综合征(PCOS)。本研究旨在探讨卡维地洛和枸橼酸克罗米芬联合用药对来曲唑诱导的PCOS大鼠抗雌激素、抗氧化和抗炎作用的可能性。方法每日给药来曲唑(1 mg/kg) 21 d诱导大鼠spcos。随后将它们分为四组,每组分别从第22-36天开始接受载药或枸橼酸克罗米芬(1 mg/kg)或卡维地洛或枸橼酸克罗米芬和卡维地洛的组合。在第35天(高架+迷宫和Y迷宫)和第36天(新物体识别)进行神经行为研究。测定大鼠额叶脑组织匀浆中抗氧化剂超氧化物歧化酶、过氧化氢酶、白细胞介素1B (IL-1B)水平及核因子-红细胞因子2相关因子2 (Nrf2)、核因子k- β (NFKB)、乙酰胆碱酯酶基因表达。结果卡维地洛联合用药均可逆转PCOS大鼠的焦虑样行为,而枸橼酸克罗米芬联合用药可改善PCOS大鼠的空间和非空间记忆障碍。卡维地洛、枸橼酸克罗米芬联合用药可提高血清SOD、过氧化氢酶浓度,降低血清IL-1B浓度。联合治疗上调NRF-2、NFKB和乙酰胆碱酯酶基因表达。结论卡维地洛联合枸橼酸克罗米芬对PCOS大鼠具有抗焦虑和改善认知功能的作用。这可能是通过卡维地洛和柠檬酸克罗米芬调节胆碱能系统和Nrf2通路,同时下调NFκB信号通路来实现的。
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