Anti-hepatopathy and anti-nephropathy activities of Taraxacum officinale in a rat model of Streptozotocin diabetes-induced hepatorenal toxicity and dyslipidemia via attenuation of oxidative stress, inflammation, apoptosis, electrolyte imbalances, and mitochondrial dysfunction

Sunday Aderemi Adelakun , Aniah Julius Akomaye , Olusegun Dare Omotoso , Olukayode Abimbola Arowosegbe
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Abstract

Diabetes and chronic liver and kidney disease are common long-term conditions worldwide. Taraxacum officinale (TOE) has many medicinal properties, due to it phytochemicals constitutions. This study investigate activities of TOE in Streptozotocin diabetes-Induced Hepatorenal toxicity. Sixty rats were randomized into groups A, B, C, D, E, and F of ten rats each (n = 10). Group normal control, group B treated with TOE, group C diabetic (DM) negative control, group D DM rats treated with TOE, group E DM rats treated with metformin (MF)], group F treated with TOE follow by STZ-diabetic). Serum lipid profile, alanine transaminase (ALT), aspartate transaminase (AST), alkaline phosphatase (ALP), Gamma-glutamyl transferase (GGT), total proteins (TP), albumin (ALB), Urea, and creatinine, electrolyte, oxidative and antioxidant enzymes, caspase 3, inflammatory cytokines, tricarboxylic acid (TCA) cycle enzymes and mitochondrial membrane potential (ΔΨm), liver and kidney histology were investigated.

Treatment with TOE ameliorated all the electrolyte disruptions in DM rats. Treatment with TOE and TOE + MF recovered caspase 3, inflammatory makers, oxidative and antioxidant enzymes in DM rats. Moreover, an increase in lipid profile, hepatic and renal functional markers, ALT, AST, ALP, GGT, TP, ALB, Urea, TCA and renal mitochondrial respiratory-chain complexes (I-IV) and ΔΨm and a decrease in creatinine clearance was recovered in DM rats by TOE and TOE + MF treatment. TOE and TOE + MF protected against hepatic and renal histological damage in DM group.

Hepatorenal toxicity was effectively ameliorated by the TOE administration. TOE might be considered as a potential protective agent against hepatorenal toxicity.

蒲公英通过减轻氧化应激、炎症、细胞凋亡、电解质失衡和线粒体功能障碍,在链脲佐菌素糖尿病诱导的肝肾毒性和血脂异常大鼠模型中具有抗肝病和抗肾病活性
糖尿病和慢性肝肾疾病是全球常见的长期疾病。蒲公英(Taraxacum officinale,TOE)因其植物化学成分而具有多种药用功效。本研究调查了蒲公英对链脲佐菌素糖尿病诱发的肝肾毒性的活性。将 60 只大鼠随机分为 A、B、C、D、E 和 F 组,每组 10 只(n = 10)。A组为正常对照组,B组为TOE治疗组,C组为糖尿病(DM)阴性对照组,D组为TOE治疗DM大鼠组,E组为二甲双胍(MF)治疗DM大鼠组,F组为STZ-糖尿病后TOE治疗组。)血清脂质概况、丙氨酸转氨酶(ALT)、天门冬氨酸转氨酶(AST)、碱性磷酸酶(ALP)、γ-谷氨酰转移酶(GGT)、总蛋白(TP)、白蛋白(ALB)、尿素和肌酐、电解质、氧化和抗氧化剂、对氧化酶和抗氧化酶、Caspase 3、炎症细胞因子、三羧酸(TCA)循环酶和线粒体膜电位(ΔΨm)、肝脏和肾脏组织学进行了研究。使用 TOE 治疗可改善 DM 大鼠的所有电解质紊乱。使用 TOE 和 TOE + MF 治疗可恢复 DM 大鼠体内的 caspase 3、炎症制造者、氧化酶和抗氧化酶。此外,TOE 和 TOE + MF 治疗后,DM 大鼠的血脂、肝肾功能指标、ALT、AST、ALP、GGT、TP、ALB、尿素、TCA 和肾线粒体呼吸链复合物(I-IV)和ΔΨm 均有所增加,肌酐清除率有所下降。TOE和TOE + MF对DM组的肝脏和肾脏组织学损伤有保护作用。TOE可被视为一种潜在的肝肾毒性保护剂。
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来源期刊
Aspects of molecular medicine
Aspects of molecular medicine Molecular Biology, Molecular Medicine
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