Baseline and recurrent exposure to the standard dose of artemisinin-based combination therapies (ACTs) induces oxidative stress and liver damage in mice (BALB/c)

IF 0.8 Q4 GASTROENTEROLOGY & HEPATOLOGY

Egyptian Liver Journal Pub Date : 2023-10-05 DOI:10.1186/s43066-023-00291-7

David Audu, Vinood B. Patel, Olufunmilayo A. Idowu, Fakilahyel M. Mshelbwala, Adewumi B. Idowu

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Abstract

Abstract Background In malaria-endemic countries, repeated intake of artemisinin-based combination therapies (ACTs) is rampant and driven by drug resistance, improper usage, and easy accessibility. Stress effects and potential liver toxicity due to the frequent therapeutic use of ACTs have not been extensively studied. Here, we investigated the effects of repeated treatment with standard doses of the commonly used ACTs artemether/lumefantrine (A/L) and artesunate-amodiaquine (A/A) on oxidative stress and liver function markers in male mice (BALB/c). Methods Forty Five mice were divided into three groups: control, A/L, and A/A. The drugs were administered three days in a row per week, and the regimen was repeated every two weeks for a total of six cycles. The levels of oxidative stress and liver function markers were measured in both plasma and liver tissue after initial (baseline) and repeated exposures for the second, third, and sixth cycles. Results Exposure to A/L or A/A caused a significant ( p < 0.001) increase in plasma malondialdehyde (MDA) levels after the first and repeated exposure periods. However, Hepatic MDA levels increased significantly ( p < 0.01) only after the sixth exposure to A/A. Following either single or repeated exposure to A/L or A/A, plasma and liver glutathione peroxidase (GPx) and catalase (CAT) activities, plasma aspartate and alanine transaminase, alkaline phosphatase activity, and bilirubin levels increased, whereas total plasma protein levels decreased significantly ( p < 0.001). Varying degrees of hepatocyte degeneration and blood vessel congestion were observed in liver tissues after a single or repeated treatment period. Conclusion Irrespective of single or repeated exposure to therapeutic doses of A/L or A/A, plasma oxidative stress and liver damage were observed. However, long-term repeated A/A exposure can led to hepatic stress. Compensatory processes involving GPx and CAT activities may help reduce the observed stress.

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基线和反复暴露于标准剂量的青蒿素为基础的联合疗法(ACTs)可诱导小鼠氧化应激和肝损伤(BALB/c)。

背景在疟疾流行国家，由于耐药、使用不当和容易获得，反复服用青蒿素类联合疗法(ACTs)的现象十分猖獗。频繁使用ACTs治疗引起的应激效应和潜在的肝毒性尚未得到广泛研究。在这里，我们研究了标准剂量的常用ACTs蒿甲醚/氨苯曲明(A/L)和青蒿琥酯-阿莫地喹(A/A)反复治疗对雄性小鼠氧化应激和肝功能标志物(BALB/c)的影响。方法45只小鼠分为对照组、A/L组和A/A组。这些药物每周连续服用三天，每两周重复一次，共六个周期。在初始(基线)和第二、第三和第六个周期的重复暴露后，在血浆和肝组织中测量氧化应激和肝功能标志物的水平。结果暴露于A/L或A/A导致显著(p <0.001)，第一次和多次暴露后血浆丙二醛(MDA)水平升高。然而，肝脏MDA水平显著升高(p <0.01)，只有在第六次暴露于A/A之后。单次或多次暴露于A/L或A/A后，血浆和肝脏谷胱甘肽过氧化物酶(GPx)和过氧化氢酶(CAT)活性、血浆天冬氨酸和丙氨酸转氨酶、碱性磷酸酶活性和胆红素水平升高，而血浆总蛋白水平显著降低(p和lt;0.001)。单次或多次治疗后，肝组织出现不同程度的肝细胞变性和血管充血。结论无论单次或多次暴露A/L或A/A治疗剂量，均可观察到血浆氧化应激和肝损伤。然而，长期重复的A/A暴露会导致肝脏应激。涉及GPx和CAT活性的代偿过程可能有助于减少观察到的应激。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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