锌通过调节 ADA/XO/UA 途径和 caspase 3 信号转导来纠正高效抗逆转录病毒治疗的 Wistar 大鼠的肝脂处理。
Zinc normalizes hepatic lipid handling via modulation of ADA/XO/UA pathway and caspase 3 signaling in highly active antiretroviral therapy-treated Wistar rats.
机构信息
Department of Medical Laboratory Sciences, Afe Babalola University, Ado-Ekiti, Ekiti State, Nigeria; The Brainwill Laboratory, Osogbo, Osun State, Nigeria; Reproductive Biology and Toxicology Research Laboratory, Oasis of Grace Hospital, Osogbo, Osun State, Nigeria.
Reproductive Biology and Toxicology Research Laboratory, Oasis of Grace Hospital, Osogbo, Osun State, Nigeria; Department of Physiology, Ladoke Akintola University of Technology, Ogbomoso, Oyo State, Nigeria.
出版信息
Chem Biol Interact. 2022 Dec 1;368:110233. doi: 10.1016/j.cbi.2022.110233. Epub 2022 Oct 27.
BACKGROUND
Although highly active antiretroviral therapy (HAART) is effective in the management of HIV, it has been reported to induce hepatic injury and non-alcoholic fatty liver (NAFLD). However, there is a lack of data on the roles of the adenosine deaminase (ADA)/xanthine oxidase (XO)/uric acid (UA) pathway and caspase 3 signaling in HAART-induced NAFLD. Also, whether or not zinc confers protection against HAART-induced NAFLD is not known.
AIM
This study evaluated the involvement of the ADA/XO/UA pathway and caspase 3 signaling in HAART-induced hepatic lipid accumulation. It also evaluated the possible protective effect of zinc in HAART-induced hepatic lipid accumulation and injury.
METHODS
Thirty two male Wistar rats (n = 8/group) were assigned into four groups namely; vehicle-treated (p.o), zinc-treated (3 mg/kg/day of elemental zinc; p.o), HAART-treated (a cocktail of 52.9 mg/kg of Efavirenz, 26.48 mg/kg of Lamivudine, and 26.48 mg/kg of Tenofovir; p.o), and HAART + zinc-treated groups. The treatment lasted for 8 weeks.
RESULTS
HAART administration led to increased body weight and hepatic weight, but unaltered hepatic organo-somatic index. HAART exposure also resulted in impaired glucose homeostasis, evidenced by increased fasting blood glucose, hyperinsulinemia, and insulin resistance (IR), increased plasma and hepatic cholesterol and triglycerides, and impaired hepatic function as depicted by elevated hepatic injury markers and reduced glycogen synthase activity and glycogen content. These findings were accompanied by increased plasma and hepatic ADA and XO activities, UA and malondialdehyde levels, inflammatory markers, and caspase 3 activities. However, HAART suppressed plasma and hepatic antioxidant defenses. Furthermore, HAART distorted hepatic histoarchitecture and reduced hepatic sinusoidal diameter. Co-administration of zinc with HAART normalized HAART-induced alterations.
CONCLUSIONS
These findings showed that downregulation of the ADA/XO/UA pathway and caspase 3 signalings may rescue the liver from HAART-induced lipid accumulation and injury.
背景
虽然高效抗逆转录病毒疗法(HAART)在 HIV 的治疗中非常有效,但它已被报道会引起肝损伤和非酒精性脂肪肝(NAFLD)。然而,关于腺苷脱氨酶(ADA)/黄嘌呤氧化酶(XO)/尿酸(UA)通路和半胱天冬酶 3 信号在 HAART 诱导的 NAFLD 中的作用的数据还很缺乏。此外,锌是否能防止 HAART 诱导的 NAFLD 也尚不清楚。
目的
本研究评估了 ADA/XO/UA 通路和半胱天冬酶 3 信号在 HAART 诱导的肝内脂质堆积中的作用。它还评估了锌在 HAART 诱导的肝内脂质堆积和损伤中的可能保护作用。
方法
将 32 只雄性 Wistar 大鼠(n=8/组)分为四组: vehicle 处理组(口服)、锌处理组(3mg/kg/天的元素锌;口服)、HAART 处理组(52.9mg/kg 的依非韦伦、26.48mg/kg 的拉米夫定和 26.48mg/kg 的替诺福韦;口服)和 HAART+锌处理组。治疗持续 8 周。
结果
HAART 给药导致体重和肝重增加,但肝器官比不变。HAART 暴露也导致葡萄糖稳态受损,表现为空腹血糖升高、高胰岛素血症和胰岛素抵抗(IR)、血浆和肝胆固醇和甘油三酯增加以及肝功能受损,表现为肝损伤标志物升高、糖原合酶活性和糖原含量降低。这些发现伴随着血浆和肝 ADA 和 XO 活性、UA 和丙二醛水平、炎症标志物和半胱天冬酶 3 活性的增加。然而,HAART 抑制了血浆和肝抗氧化防御。此外,HAART 改变了肝组织学结构并降低了肝窦直径。锌与 HAART 联合给药可使 HAART 诱导的改变正常化。
结论
这些发现表明,ADA/XO/UA 通路和半胱天冬酶 3 信号的下调可能使肝脏免受 HAART 诱导的脂质堆积和损伤。
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