GSK-3β as a Potential Coordinator of Anabolic and Catabolic Pathways in Hepatitis C Virus Insulin Resistance.

IF 3.2 4区 医学 Q3 VIROLOGY Intervirology Pub Date : 2024-01-01 Epub Date: 2023-12-15 DOI:10.1159/000535787
Gokul C Das, F Blaine Hollinger
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引用次数: 0

Abstract

Introduction: Chronic hepatitis C infection can result in insulin resistance (IR). We have previously shown that it occurs through the interaction of pathways for glucose homeostasis, insulin signaling, and autophagy. But it is not known how soon the pathways are activated and how IR is related to the signals generated by catabolic and anabolic conditions occurring in infected cells. We have extended our studies to a cell culture system mimicking acute infection and to downstream pathways involving energy-sensor AMPK and nutrient-sensor mTOR that are active in catabolic and anabolic processes within the infected cells.

Methods: Huh7 liver cells in culture were infected with hepatitis C virus (HCV). We performed proteomics analysis of key proteins in infected cells by Western blotting and IP experiments, with or without IFNα exposure as a component of conventional therapeutic strategy.

Results: We present evidence that (a) IRS-1 Ser312, Beclin-1, protein conjugate Atg12-Atg5 or GS Ser641 are up-regulated early in infection presumably by activating the same pathways as utilized for persistent infection; (b) Bcl-XL, an inhibitor of both autophagy and apoptosis, is present in a core complex with IRS-1 Ser312 and Beclin-1 during progression of IR; (c) AMPK level remains about the same in infected cells where it is activated by phosphorylation at Thr172 concomitant with increased autophagy, a hallmark of catabolic conditions; (d) an mTOR level that promotes anabolism is increased rather than decreased under an expanded autophagy; (e) hypophosphorylation of translational repressor 4E-BP1 downstream of mTOR is suggestive of reduced protein synthesis; and (f) β-catenin, is up-regulated but not phosphorylated suggesting indirectly our previous contention that its kinase, GSK-3β, is mostly in an inactive state.

Conclusion: We report that in the development of IR following chronic infection, anabolic and catabolic pathways are activated early, and the metabolic interaction occurs possibly in a core complex with IRS-1 Ser312, Beclin-1, and autophagy inhibitor Bcl-XL. Induction of autophagy is usually controlled by a two-edged mechanism acting in opposition under anabolic and catabolic conditions by AMPK/mTOR/4E-BP1 pathway with GSK-3β-mediated feedback loops. However, we have observed an up-regulation of mTOR along with an up-regulation of AMPK caused by HCV infection is a deviation from the normal scenario described above which might be of therapeutic interest.

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GSK-3β 是丙型肝炎病毒胰岛素抵抗中合成代谢和分解代谢途径的潜在协调者。
简介:慢性 HCV 感染会通过葡萄糖平衡、胰岛素信号传导和自噬等途径的相互作用导致胰岛素抵抗(IR)。目前尚不清楚这些途径多久会被激活,以及胰岛素抵抗与感染细胞内分解代谢和合成代谢条件产生的信号有何关系。我们将研究扩展到模拟急性感染的细胞培养系统,以及涉及能量传感器 AMPK 和营养传感器 mTOR 的下游通路,这些通路在感染细胞内的分解代谢和合成代谢过程中十分活跃。方法:Huh7 肝细胞感染了 HCV,我们通过 Western 印迹和 IP 实验对感染细胞中的关键蛋白进行了蛋白质组学分析:结果:我们发现,IRS-1 Ser312、Beclin-1、蛋白共轭物 Atg12-Atg5 或 GS Ser641 在感染早期通过激活用于持续感染的相同途径而上调;Bcl-XL是自噬和细胞凋亡的抑制剂,在IR进展过程中与IRS-1 Ser312和Beclin-1形成核心复合物;AMPK水平在感染细胞中保持不变,它通过Thr172处的磷酸化被激活,同时自噬增加,这是分解代谢的标志;mTOR下游的翻译抑制因子4E-BP1磷酸化不足,表明蛋白质合成减少;β-catenin上调但未磷酸化,间接表明我们之前的论点,即其激酶GSK-3β大多处于非活性状态。讨论/结论:我们报告说,在慢性感染后IR的发展过程中,合成代谢和分解代谢途径在早期就被激活,代谢相互作用可能发生在与IRS-1 Ser312、Beclin-1和自噬抑制剂BcL-XL的核心复合物中。自噬的诱导通常由一个双刃机制控制,在合成代谢和分解代谢条件下,AMPK/mTOR/4E-BP1 通路与 GSK-3β 介导的回馈回路对立作用。然而,我们观察到,HCV 感染导致的 mTOR 上调和 AMPK 上调偏离了上述正常情况,这可能具有治疗意义。
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来源期刊
Intervirology
Intervirology 医学-病毒学
CiteScore
5.40
自引率
0.00%
发文量
13
审稿时长
6-12 weeks
期刊介绍: ''Intervirology'' covers progress in both basic and clinical virus research, and aims to provide a forum for the various disciplines within virology. Issues publishing original papers alternate with thematic issues, focusing on clearly defined topics. This thematic concentration serves to make timely reviews, research reports and controversy easily accessible to both specialists in the field and those who want to keep track of the latest developments outside their own area of interest. In addition to original papers, regular issues publish short communications and letters to the editor to provide readers with a forum for the exchange of ideas and comments. The scope encompasses work on the molecular biology of human and animal viruses, including genome organization and regulation, and the structure and function of viral proteins. The pathogenesis, immunology, diagnosis, epidemiology, prophylaxis and therapy of viral diseases are considered.
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