Low-dose quercetin at 25 mg/kg ameliorates dolutegravir-lamivudine-tenofovirdisoproxilfumarate-inducedcardio-hepato-renal toxicities in Wistar rats

Innocent A. Edagha, Blessing C. Akpan, David O. Edem, Moses A. Ataben, Blessing U. Bassey, Royal S. Itama, Deborah C. Evogor
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Abstract

Combination antiretroviral therapies (cARTs) are linked with multiple-organ system (MOS) toxicities in laboratory animals, and in humans undertaking treatment for HIV/AIDS. The ameliorative potential of low-dose quercetin following cART-associated MOS-toxicities in cardio-hepato-renal organs was evaluated in in vivo model. Oral administration of cART (Dolutegravir 50 mg, Lamivudine 300 mg and Tenofovir disoproxil fumarate 300 mg [DLT]) at 9.29 mg/kg, was challenged against low-dose quercetin 25 mg/kg body weight (bw) in Wistar rats. Group 1, the normal control (NC) received distilled water (5 mL), while groups 2 to 4 received quercetin (25 mg), DLT (9.29 mg), and DLT + quercetin (9.29 mg + 25 mg respectively), per kg bw. All administrations lasted for 14 days, and thereafter animals were humanely sacrificed after intraperitoneal anesthesia injection with 100 mg ketamine /5 mg xylazine per kg bw followed by cervical dislocation. Blood and organs were harvested for analyses using standard protocols. The serum concentrations of lipid parameters [total cholesterol, triglycerides, LDL-cholesterol, and VLDL-cholesterol], liver biomarkers (total-bilirubin, direct-bilirubin, and transaminases], and kidney biomarkers [urea and creatinine] were significantly increased (p < 0.05) while electrolytes (Na+, K+, Cl− and HCO3−) were significantly decreased (p < 0.05) in DLT group but improved in DLT + Q group. Histopathology demonstrated distorted myocytes, hepatocytes and renal tubules, fatty liver with vacuolization, dystrophied glomeruli and distorted renal interstitium in DLT group, compared with normal appearing histoarchitectural features in NC and DLT + Q groups. In conclusion, oral administration of low-dose quercetin (25 mg/kg) ameliorated cART-associated cardio-hepato-renal toxicities in rats, improving their biomarkers and histoarchitecture.
25 毫克/千克的小剂量槲皮素可改善多罗替韦-拉米夫定-替诺福韦酯-异丙嗪富马酸盐诱发的 Wistar 大鼠心、肝、肾毒性反应
在实验动物和接受艾滋病毒/艾滋病治疗的人类中,抗逆转录病毒联合疗法(cARTs)与多器官系统(MOS)毒性有关。我们在体内模型中评估了小剂量槲皮素对与 cART 相关的心肝肾器官多器官毒性的改善潜力。在 Wistar 大鼠体内口服 9.29 毫克/千克的 cART(多托曲韦 50 毫克、拉米夫定 300 毫克和富马酸替诺福韦二吡呋酯 300 毫克 [DLT])与低剂量槲皮素 25 毫克/千克体重(bw)。第 1 组为正常对照组(NC),接受蒸馏水(5 毫升);第 2 至第 4 组分别接受槲皮素(25 毫克)、DLT(9.29 毫克)和 DLT + 槲皮素(9.29 毫克 + 25 毫克)。所有给药持续 14 天,然后每公斤体重腹腔注射 100 毫克氯胺酮/5 毫克甲苯噻嗪麻醉动物,再进行颈椎脱臼,最后人道处死。按照标准方案采集血液和器官进行分析。血清中血脂参数[总胆固醇、甘油三酯、低密度脂蛋白胆固醇和超低密度脂蛋白胆固醇]、肝脏生物标志物(总胆红素、直接胆红素和转氨酶)和肾脏生物标志物[尿素和肌酐]的浓度均显著增加(p < 0.05),而电解质(Na+、K+、Cl- 和 HCO3-)在 DLT 组明显下降(p < 0.05),但在 DLT + Q 组有所改善。组织病理学显示,DLT 组的肌细胞、肝细胞和肾小管变形,脂肪肝伴空泡化,肾小球萎缩,肾间质变形,而 NC 组和 DLT + Q 组的组织结构特征正常。总之,口服小剂量槲皮素(25 毫克/千克)可改善大鼠与 cART 相关的心肝肾毒性,改善其生物标志物和组织结构。
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来源期刊
自引率
0.00%
发文量
18
审稿时长
13 weeks
期刊介绍: Clinical Phytoscience is an international, peer-reviewed, interdisciplinary, and open access journal publishing high quality research articles on clinical evidence and use of medicinal plants in the development of efficient and well tolerated phytotherapy. Clinical Phytoscience focuses on phytotherapy, looking at proof of concept, efficacy and safety, to be established “at eye level” compared to pharmacotherapy. The emphasis lies on application oriented topics (efficacy and safety of phytotherapy in a specific indication, including its need and acceptance by the patient). The scientific results published in the journal should contribute to the recovery and maintenance of human health by phytotherapy. Clinical Phytoscience will publish high-quality evidence-based clinical studies and relevant pharmacological studies. Key areas of interest are: -Upper and lower airways, ENT and pneumology -Gynecology -Urology -Nephrology Pediatrics -Intestinal tract -Hepatology -Diabetes/metabolic Syndrome -Immunology and microbiology -Hygiene -Analytics
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