PPARα-ERRα串扰减轻代谢功能障碍相关的脂肪变性肝病进展。

IF 10.8 1区医学 Q1 ENDOCRINOLOGY & METABOLISM

Metabolism: clinical and experimental Pub Date : 2024-12-30 DOI:10.1016/j.metabol.2024.156128

Milton Boaheng Antwi , Sander Lefere , Dorien Clarisse , Lisa Koorneef , Anneleen Heldens , Louis Onghena , Kylian Decroix , Daria Fijalkowska , Jonathan Thommis , Madeleine Hellemans , Anne Hoorens , Anja Geerts , Lindsey Devisscher , Karolien De Bosscher

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引用次数: 0

摘要

背景和目的：代谢功能障碍相关脂肪变性肝病（MASLD）是世界上最常见的肝脏疾病，其发病率持续上升。迫切需要更有效的治疗策略。我们研究了参与肝脏能量代谢的两个关键核受体，过氧化物酶体增殖体激活受体α (PPARα)和雌激素相关受体α (ERRα)，如何改善MASLD。方法：在短期和长期西方饮食加果糖模型，以及糖尿病背景链脲佐菌素-西方饮食模型（STZ-WD）中给予PPARα激动剂pemafbrate和/或ERRα逆激动剂C29。分析肝脏和脂肪组织形态、组织学样品、血清代谢物、RNA和蛋白质水平，并进行扫描电镜检查。此外，我们对健康、MASLD和MASH的人肝脏进行了基于细胞的检测、免疫组织化学和免疫荧光染色，使用光和超分辨率共聚焦显微镜。结果：在所有小鼠模型中，配体组合的功效都得到了突出的体现，即肝脏脂肪变性减少，同时在两种长期模型中，体重、炎症和纤维化都得到了改善。此外，在STZ-WD小鼠模型中，肿瘤形成被阻止。基于细胞的实验表明，ERRα抑制PPARα的活性，解释了为什么ERRα阻断可改善炎症和脂质代谢基因谱，并增强降脂作用。互补RNA测序和鸟枪蛋白组学，结合富集分析，共同确定下调的血清淀粉样蛋白A1/A2是联合治疗有效性的基本成分。MASLD/MASH患者肝脏显示PPARα降低，ERRα水平升高，支持肝细胞核NR串扰中断。结论：我们的研究支持双核受体靶向，同时增加PPARα和降低ERRα活性，可能是一种可行的治疗MASLD的新策略。影响和启示：我们的研究引入了一种新的治疗策略，通过同时增加PPARα活性，同时降低ERRα活性来治疗MASLD。由于PPARα激动剂已经在III期临床试验中进行了测试，ERRα配体/调节剂需要进一步的（临床）开发，以使我们的发现适用于MASLD患者和医生。

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PPARα-ERRα crosstalk mitigates metabolic dysfunction-associated steatotic liver disease progression

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PPARα-ERRα crosstalk mitigates metabolic dysfunction-associated steatotic liver disease progression

Background and aims

Metabolic dysfunction-associated steatotic liver disease (MASLD), the most prevalent liver disease worldwide, continues to rise. More effective therapeutic strategies are urgently needed. We investigated how targeting two key nuclear receptors involved in hepatic energy metabolism, peroxisome proliferator-activated receptor alpha (PPARα) and estrogen-related receptor alpha (ERRα), ameliorates MASLD.

Methods

The PPARα agonist pemafibrate and/or ERRα inverse agonist C29 were administered in a short- and long-term Western diet plus fructose model, and a diabetic-background streptozotocin-Western diet model (STZ-WD). Liver and adipose tissue morphology, histological samples, serum metabolites, RNA and protein levels were analysed and scanning electron microscopy was performed. In addition, we performed cell-based assays and immunohistochemistry and immunofluorescence stainings with light and super-resolution confocal microscopy of healthy, MASLD and MASH human livers.

Results

The ligand combinations' efficacy was highlighted by reduced liver steatosis across all mouse models, alongside improvements in body weight, inflammation, and fibrosis in both long-term models. Additionally, tumour formation was prevented in the STZ-WD mice model. Cell-based assays demonstrated that ERRα inhibits PPARα's activity, explaining why ERRα blockage improves inflammatory and lipid metabolism gene profiles and enhances lipid-lowering effects. Complementary RNA sequencing and shotgun proteomics, combined with enrichment analysis, jointly identified downregulated serum amyloid A1/A2 as essential components underlying the combination treatment's effectiveness. MASLD/MASH patient livers showed reduced PPARα and increased ERRα levels supporting disrupted NR crosstalk in the hepatocyte nucleus.

Conclusion

Our study supports that dual nuclear receptor targeting, which simultaneously increases PPARα and diminishes ERRα activity, may represent a viable novel strategy against MASLD.

Impact and implications

Our research introduces a novel therapeutic strategy against MASLD by simultaneously increasing PPARα activity while diminishing ERRα activity. With PPARα agonists already tested in phase III clinical trials, ERRα ligands/modulators need further (clinical) development to make our findings applicable to both MASLD patients and physicians.

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来源期刊

Metabolism: clinical and experimental 医学-内分泌学与代谢

CiteScore

18.90

自引率

3.10%

发文量

310

审稿时长

16 days

期刊介绍： Metabolism upholds research excellence by disseminating high-quality original research, reviews, editorials, and commentaries covering all facets of human metabolism. Consideration for publication in Metabolism extends to studies in humans, animal, and cellular models, with a particular emphasis on work demonstrating strong translational potential. The journal addresses a range of topics, including: - Energy Expenditure and Obesity - Metabolic Syndrome, Prediabetes, and Diabetes - Nutrition, Exercise, and the Environment - Genetics and Genomics, Proteomics, and Metabolomics - Carbohydrate, Lipid, and Protein Metabolism - Endocrinology and Hypertension - Mineral and Bone Metabolism - Cardiovascular Diseases and Malignancies - Inflammation in metabolism and immunometabolism