Insulin-degrading enzyme inhibition increases the unfolded protein response and favours lipid accumulation in the liver

IF 6.8 2区医学 Q1 PHARMACOLOGY & PHARMACY British Journal of Pharmacology Pub Date : 2024-05-29 DOI:10.1111/bph.16436

Marine Andres, Nathalie Hennuyer, Khamis Zibar, Marie Bicharel-Leconte, Isabelle Duplan, Emmanuelle Enée, Emmanuelle Vallez, Adrien Herledan, Anne Loyens, Bart Staels, Benoit Deprez, Peter van Endert, Rebecca Deprez-Poulain, Steve Lancel

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Abstract

Background and Purpose

Nonalcoholic fatty liver disease refers to liver pathologies, ranging from steatosis to steatohepatitis, with fibrosis ultimately leading to cirrhosis and hepatocellular carcinoma. Although several mechanisms have been suggested, including insulin resistance, oxidative stress, and inflammation, its pathophysiology remains imperfectly understood. Over the last decade, a dysfunctional unfolded protein response (UPR) triggered by endoplasmic reticulum (ER) stress emerged as one of the multiple driving factors. In parallel, growing evidence suggests that insulin-degrading enzyme (IDE), a highly conserved and ubiquitously expressed metallo-endopeptidase originally discovered for its role in insulin decay, may regulate ER stress and UPR.

Experimental Approach

We investigated, by genetic and pharmacological approaches, in vitro and in vivo, whether IDE modulates ER stress-induced UPR and lipid accumulation in the liver.

Key Results

We found that IDE-deficient mice display higher hepatic triglyceride content along with higher inositol-requiring enzyme 1 (IRE1) pathway activation. Upon induction of ER stress by tunicamycin or palmitate in vitro or in vivo, pharmacological inhibition of IDE, using its inhibitor BDM44768, mainly exacerbated ER stress-induced IRE1 activation and promoted lipid accumulation in hepatocytes, effects that were abolished by the IRE1 inhibitors 4μ8c and KIRA6. Finally, we identified that IDE knockout promotes lipolysis in adipose tissue and increases hepatic CD36 expression, which may contribute to steatosis.

Conclusion and Implications

These results unravel a novel role for IDE in the regulation of ER stress and development of hepatic steatosis. These findings pave the way to innovative strategies modulating IDE to treat metabolic diseases.

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抑制胰岛素降解酶会增加未折叠蛋白反应，有利于肝脏中的脂质积累。

背景和目的：非酒精性脂肪肝是指从脂肪变性到脂肪性肝炎的肝脏病变，其纤维化最终导致肝硬化和肝细胞癌。尽管已提出了包括胰岛素抵抗、氧化应激和炎症在内的几种机制，但对其病理生理学的理解仍不完善。在过去十年中，由内质网（ER）应激引发的未折叠蛋白反应（UPR）功能失调成为多种驱动因素之一。与此同时，越来越多的证据表明，胰岛素降解酶（IDE）--一种高度保守且普遍表达的金属内肽酶，最初因其在胰岛素降解中的作用而被发现，可能会调节ER应激和UPR：实验方法：我们通过遗传学和药理学方法，在体外和体内研究了 IDE 是否调节 ER 应激诱导的 UPR 和肝脏中的脂质积累：我们发现，IDE缺陷小鼠的肝脏甘油三酯含量较高，同时肌醇需要酶1（IRE1）通路活化程度较高。在体外或体内使用妥卡霉素或棕榈酸酯诱导ER应激时，使用IDE抑制剂BDM44768对IDE进行药理抑制，主要会加剧ER应激诱导的IRE1活化并促进肝细胞中的脂质积累，而IRE1抑制剂4μ8c和KIRA6可消除这些效应。最后，我们发现 IDE 基因敲除会促进脂肪组织的脂肪分解，增加肝脏 CD36 的表达，这可能会导致脂肪变性：这些结果揭示了 IDE 在调节 ER 应激和肝脏脂肪变性中的新作用。这些发现为调控 IDE 治疗代谢性疾病的创新策略铺平了道路。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

British Journal of Pharmacology 医学-药学

CiteScore

15.40

自引率

12.30%

发文量

270

审稿时长

2.0 months

期刊介绍： The British Journal of Pharmacology (BJP) is a biomedical science journal offering comprehensive international coverage of experimental and translational pharmacology. It publishes original research, authoritative reviews, mini reviews, systematic reviews, meta-analyses, databases, letters to the Editor, and commentaries. Review articles, databases, systematic reviews, and meta-analyses are typically commissioned, but unsolicited contributions are also considered, either as standalone papers or part of themed issues. In addition to basic science research, BJP features translational pharmacology research, including proof-of-concept and early mechanistic studies in humans. While it generally does not publish first-in-man phase I studies or phase IIb, III, or IV studies, exceptions may be made under certain circumstances, particularly if results are combined with preclinical studies.