ASPP2 deficiency attenuates lipid accumulation through the PPARγ pathway in alcoholic liver injury.

IF 5.3 2区 医学 Q2 CELL BIOLOGY Cell Biology and Toxicology Pub Date : 2024-11-22 DOI:10.1007/s10565-024-09925-x
Ying Zhang, Xingzhong Miao, Fang Liu, Honglin Shi, Dexi Chen, Yu Chen, Yingmin Ma, Hongbo Shi
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Abstract

The initial stage of alcoholic liver disease (ALD) is hepatic steatosis. Recent studies have highlighted a possible role for Apoptosis-stimulating protein 2 of p53 (ASPP2) in regulating hepatic lipid metabolism in nonalcoholic fatty liver (NAFLD). However, whether ASPP2 regulates alcohol-induced lipid accumulation and its mechanisms remain unclear. To explore that, we establish an alcoholic liver injury model in vivo and in vitro. The clinical specimens were collected from liver tissues of patients with alcoholic liver disease. Lipid metabolism was detected by HE staining, oil red O staining and qPCR; and ASPP2-peroxisome proliferator-activated receptor γ (PPARγ) signaling pathways were detected by western blot and immunohistochemical staining. We found that both ASPP2 and PPARγ expression increased in patients and mouse models with ALD. We also discovered the reduction of ASPP2 significantly inhibited the expression of PPARγ and alleviated alcohol-induced hepatic lipid accumulation and liver injury in vivo and in vitro. Mechanistically, the PPARγ agonist reversed the protective effect of ASPP2 downregulation on hepatic steatosis and liver injury, while the opposite results were observed using PPARγ inhibitor. In conclusion, ASPP2 exacerbates ethanol-induced lipid accumulation and hepatic injury by upregulating the PPARγ signaling pathway, thus promoting the occurrence and development of ALD.

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缺乏 ASPP2 可通过 PPARγ 途径减轻酒精性肝损伤中的脂质积累。
酒精性肝病(ALD)的初始阶段是肝脂肪变性。最近的研究强调了 p53 的凋亡刺激蛋白 2(ASPP2)在非酒精性脂肪肝(NAFLD)中调节肝脂代谢的可能作用。然而,ASPP2 是否调控酒精诱导的脂质蓄积及其机制仍不清楚。为了探讨这一问题,我们在体内和体外建立了酒精性肝损伤模型。临床标本采集自酒精性肝病患者的肝组织。通过HE染色、油红O染色和qPCR检测脂质代谢;通过Western印迹和免疫组化染色检测ASPP2-过氧化物酶体增殖激活受体γ(PPARγ)信号通路。我们发现,在 ALD 患者和小鼠模型中,ASPP2 和 PPARγ 的表达均有所增加。我们还发现,减少 ASPP2 能显著抑制 PPARγ 的表达,减轻酒精诱导的体内和体外肝脂质蓄积和肝损伤。从机理上讲,PPARγ 激动剂逆转了 ASPP2 下调对肝脏脂肪变性和肝损伤的保护作用,而 PPARγ 抑制剂则观察到相反的结果。总之,ASPP2 通过上调 PPARγ 信号通路加剧乙醇诱导的脂质积累和肝损伤,从而促进 ALD 的发生和发展。
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来源期刊
Cell Biology and Toxicology
Cell Biology and Toxicology 生物-毒理学
CiteScore
9.90
自引率
4.90%
发文量
101
审稿时长
>12 weeks
期刊介绍: Cell Biology and Toxicology (CBT) is an international journal focused on clinical and translational research with an emphasis on molecular and cell biology, genetic and epigenetic heterogeneity, drug discovery and development, and molecular pharmacology and toxicology. CBT has a disease-specific scope prioritizing publications on gene and protein-based regulation, intracellular signaling pathway dysfunction, cell type-specific function, and systems in biomedicine in drug discovery and development. CBT publishes original articles with outstanding, innovative and significant findings, important reviews on recent research advances and issues of high current interest, opinion articles of leading edge science, and rapid communication or reports, on molecular mechanisms and therapies in diseases.
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