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Safety Assessment of Ubiquinol Acetate: Subchronic Toxicity and Genotoxicity Studies

机译:乙酸泛醇的安全性评估:慢性毒性和遗传毒性研究

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摘要

Coenzyme Q10 (CoQ10) is a lipid soluble, endogenous antioxidant present at highest levels in the heart followed by the kidney and liver. The reduced CoQ10 ubiquinol is well known for its chemical instability and low bioavailability. The present study was designed to synthesize ubiquinol acetate, which is more stable and biologically active, and further evaluate its safety and genotoxic potential. Synthesized ubiquinol acetate showed better stability than that of ubiquinol at the end of 3 months. In vitro genotoxicity studies (AMES test, in vitro micronucleus and chromosomal aberration) showed ubiquinol acetate as nongenotoxic with no clastogenic or aneugenic effects at high dose of 5000 and 62.5 μg/mL, respectively. In subchronic toxicity study, ubiquinol acetate was administered orally to Sprague Dawley rats at 150, 300, and 600 mg/kg/day for 90 days. No treatment related adverse effects were observed in males at 600 mg/kg/day; however, females showed treatment related increase in AST and ALT with small focal irregular white-yellow spots in liver on gross necropsy examination. Histopathological evaluation revealed hepatocellular necrosis in high dose females which was considered as adverse. Based on the results, the No-Observed-Adverse-Effect Level (NOAEL) of ubiquinol acetate in males and females was determined as 600 and 300 mg/kg/day, respectively.
机译:辅酶Q10(CoQ10)是脂溶性内源性抗氧化剂,在心脏中含量最高,其次是肾脏和肝脏。降低的辅酶Q10泛醇以其化学不稳定性和低生物利用度而闻名。本研究旨在合成更稳定和具有生物活性的乙酸泛醇,并进一步评估其安全性和遗传毒性。合成的乙酸泛醇在3个月末显示出比泛醇更好的稳定性。体外遗传毒性研究(AMES测试,体外微核和染色体畸变)显示乙酸泛醇非遗传毒性,分别在5000和62.5μg/ mL的高剂量下无消融或生瘤作用。在亚慢性毒性研究中,以150、300和600 mg / kg / day的剂量向Sprague Dawley大鼠口服醋酸泛醇90天。男性在600 mg / kg / day时未观察到与治疗相关的不良反应;但是,在尸检中,女性显示出与治疗相关的AST和ALT升高,肝脏中有小的局灶性不规则白黄点。组织病理学评估显示高剂量女性的肝细胞坏死被认为是不利的。根据该结果,确定男性和女性的乙酸泛醇的未观察到不良作用水平(NOAEL)分别为600和300 mg / kg / day。

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