Effects of alfa lipoic acid and coenzyme Q10 treatment on AFB1-induced oxidative, inflammatory, and DNA damages in rats

IF 2.6 4区 医学 Q2 PHARMACOLOGY & PHARMACY
Ghadeer M. Albadrani , Ahmed E. Altyar , Osama A. Kensara , Mohie A.M. Haridy , Mohamed Sayed Zaazouee , Alaa Ahmed Elshanbary , Amany A. Sayed , Mohamed M. Abdel-Daim
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引用次数: 0

Abstract

Food contamination with Aflatoxin B1 (AFB1) is a worldwide concern that adversely affects animal and human health. The study aimed to evaluate the protective effect of alpha lipoic acid (ALA) and/or co-enzyme Q10 (CQ10) against the harmful effects of AFB1 on the liver and kidneys. Fifty-six mature male Wistar Albino rats (180–200 g) were divided into seven groups, each with eight rats: (1) saline was given as a control, (2) ALA (100 mg/kg bw/day) was given by stomach gavage for fifteen days, and (3) CQ10 (10 mg/kg bw/day) was given by stomach gavage for fifteen days. Group (4) orally given AFB1 (2.5 mg/kg bw) on days 12th and 14th, (5) received AFB1 and ALA, (6) received AFB1 and CQ10, and (7) received AFB1, ALA, and CQ10, as previously described in the ALA, CQ10, and AFB1 groups. After the exposure to AFB1, a significant increase in liver markers (AST, ALT, ALP, and LDH) and renal function tests (BUN and creatinine) was observed compared with the control. ALA and/or CQ10 significantly reduced enzymes of liver and renal functions, as compared with AFB1. AFB1 exposure threw off the balance between oxidants and antioxidants. Still, ALA and/or CQ10 made oxidative stress (MDA, NO, and 8-OHdG) much lower and antioxidant activities (GSH, GSH-Px, SOD, and CAT) much higher. When we used the two together, the activities matched the control levels. Interestingly, this study shows that ALA and CQ10 significantly lowered IL-1β, IL-6, and TNF-α levels compared to the control values when used together after AFB1 exposure caused robust inflammation. Some CQ10 treatment parameters significantly outperformed those of ALA. ALA and CQ10 together worked better than either one alone to protect against AFB1-induced toxicity in the hepatic and renal parenchyma in terms of reducing inflammation, preventing DNA damage, and fighting free radicals.

Abstract Image

阿法硫辛酸和辅酶 Q10 对 AFB1 诱导的大鼠氧化、炎症和 DNA 损伤的影响
黄曲霉毒素 B1(AFB1)污染食品是一个全球关注的问题,对动物和人类健康造成了不利影响。本研究旨在评估α-硫辛酸(ALA)和/或辅酶 Q10(CQ10)对 AFB1 对肝脏和肾脏有害影响的保护作用。将 56 只成年雄性 Wistar Albino 大鼠(180-200 克)分为 7 组,每组 8 只:(1) 以生理盐水作为对照;(2) 口服 ALA(100 毫克/千克体重/天)15 天;(3) 口服 CQ10(10 毫克/千克体重/天)15 天。第 12 天和第 14 天,(4) 组口服 AFB1(2.5 毫克/千克体重);(5) 组口服 AFB1 和 ALA;(6) 组口服 AFB1 和 CQ10;(7) 组口服 AFB1、ALA 和 CQ10。与对照组相比,暴露于 AFB1 后,观察到肝脏指标(AST、ALT、ALP 和 LDH)和肾功能测试(BUN 和肌酐)显著增加。与 AFB1 相比,ALA 和/或 CQ10 能明显降低肝功能和肾功能酶的含量。暴露于 AFB1 会破坏氧化剂和抗氧化剂之间的平衡。尽管如此,ALA 和/或 CQ10 仍大大降低了氧化应激(MDA、NO 和 8-OHdG),提高了抗氧化活性(GSH、GSH-Px、SOD 和 CAT)。当我们同时使用这两种抗氧化剂时,抗氧化活性与对照组水平相当。有趣的是,这项研究表明,在暴露于 AFB1 引起强烈炎症后,ALA 和 CQ10 一起使用时,IL-1β、IL-6 和 TNF-α 的水平与对照值相比明显降低。CQ10 的一些治疗参数明显优于 ALA。在减轻炎症、防止DNA损伤和对抗自由基方面,ALA和CQ10在保护肝脏和肾脏实质免受AFB1诱导的毒性方面的作用优于单独使用其中一种。
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来源期刊
Toxicon
Toxicon 医学-毒理学
CiteScore
4.80
自引率
10.70%
发文量
358
审稿时长
68 days
期刊介绍: Toxicon has an open access mirror Toxicon: X, sharing the same aims and scope, editorial team, submission system and rigorous peer review. An introductory offer Toxicon: X - full waiver of the Open Access fee. Toxicon''s "aims and scope" are to publish: -articles containing the results of original research on problems related to toxins derived from animals, plants and microorganisms -papers on novel findings related to the chemical, pharmacological, toxicological, and immunological properties of natural toxins -molecular biological studies of toxins and other genes from poisonous and venomous organisms that advance understanding of the role or function of toxins -clinical observations on poisoning and envenoming where a new therapeutic principle has been proposed or a decidedly superior clinical result has been obtained. -material on the use of toxins as tools in studying biological processes and material on subjects related to venom and antivenom problems. -articles on the translational application of toxins, for example as drugs and insecticides -epidemiological studies on envenoming or poisoning, so long as they highlight a previously unrecognised medical problem or provide insight into the prevention or medical treatment of envenoming or poisoning. Retrospective surveys of hospital records, especially those lacking species identification, will not be considered for publication. Properly designed prospective community-based surveys are strongly encouraged. -articles describing well-known activities of venoms, such as antibacterial, anticancer, and analgesic activities of arachnid venoms, without any attempt to define the mechanism of action or purify the active component, will not be considered for publication in Toxicon. -review articles on problems related to toxinology. To encourage the exchange of ideas, sections of the journal may be devoted to Short Communications, Letters to the Editor and activities of the affiliated societies.
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