NORAD exacerbates metabolic dysfunction-associated steatotic liver disease development via the miR-511-3p/Rock2 axis and inhibits ubiquitin-mediated degradation of ROCK2

IF 10.8 1区医学 Q1 ENDOCRINOLOGY & METABOLISM

Metabolism: clinical and experimental Pub Date : 2024-12-20 DOI:10.1016/j.metabol.2024.156111

Xu Zhang , Tianxing Chen , Zhenhan Li , Lingfeng Wan , Zhihang Zhou , Ying Xu , Dong Yan , Wei Zhao , Hao Chen

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Abstract

Background & aims

Abnormal regulation of lncRNA is strongly linked to metabolic dysfunction-associated steatotic liver disease (MASLD). However, the precise molecular mechanisms remain unclear. This study explores the roles of noncoding RNA activated by DNA damage (NORAD)/miR-511-3p/Rho-associated protein kinase 2 (Rock2) axis and the NORAD/ROCK2 interaction in the development of MASLD.

Methods

In vitro and in vivo models of MASLD were created using high-fat diet-fed mice and free fatty acid (FFA)-treated hepatocytes. To examine the relationships between NORAD, miR-511-3p, and ROCK2, we employed bioinformatics, luciferase assays, RNA immunoprecipitation, and biotinylated NORAD pull-down assays. MASLD progression was assessed based on food intake, energy expenditure, insulin resistance, hepatic steatosis, inflammation, white fat growth, and liver fibrosis.

Results

NORAD and ROCK2 were upregulated, while miR-511-3p was downregulated in MASLD liver tissues and FFA-treated hepatocytes. Mechanistically, NORAD competitively interacted with miR-511-3p to modulate Rock2 mRNA expression, and directly stabilized ROCK2 protein by abrogating its ubiquitination degradation. Functionally, liver-specific knockdown of NORAD or overexpression of miR-511-3p significantly slowed MASLD progression. Overexpression of NORAD or ROCK2 partially reversed miR-511-3p-induced inhibition of MASLD. Additionally, ROCK2 knockdown attenuated NORAD-induced worsening of MASLD. Moreover, overexpressing NORAD or ROCK2 or interfering miR-511-3p influenced resmetirom treatment to suppress MASLD development. Finally, metabolic changes in liver driven by the NORAD/miR-511-3p/Rock2 axis and NORAD/ROCK2 interaction also influenced white adipose growth, pancreatic β-cell dedifferentiation, and liver fibrosis.

Conclusions

The NORAD/miR-511-3p/Rock2 axis and the NORAD/ROCK2 interaction play critical roles in MASLD progression, identifying potential therapeutic targets for its treatment.

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NORAD通过miR-511-3p/Rock2轴加剧代谢功能障碍相关的脂肪变性肝病的发展，并抑制泛素介导的Rock2降解。

背景与目的：长链非编码rna的异常表达与代谢功能障碍相关的脂肪变性肝病（MASLD）密切相关。然而，确切的分子机制尚不清楚。本研究探讨了DNA损伤激活的非编码RNA (NORAD)/miR-511-3p/ rho相关蛋白激酶2 （Rock2）轴和NORAD/ Rock2相互作用在MASLD发展中的作用。方法：采用高脂饲料喂养小鼠和游离脂肪酸（FFA）处理的肝细胞建立MASLD体外和体内模型。为了检验NORAD、miR-511-3p和ROCK2之间的关系，我们采用了生物信息学、荧光素酶测定、RNA免疫沉淀和生物素化NORAD拉下测定。根据食物摄入、能量消耗、胰岛素抵抗、肝脂肪变性、炎症、白色脂肪生长和肝纤维化来评估MASLD的进展。结果：在MASLD肝组织和fa处理的肝细胞中，NORAD和ROCK2上调，miR-511-3p下调。在机制上，NORAD与miR-511-3p竞争性地相互作用以调节Rock2 mRNA的表达，并通过消除其泛素化降解直接稳定Rock2蛋白。功能上，肝脏特异性敲低NORAD或过表达miR-511-3p可显著减缓MASLD的进展。NORAD或ROCK2的过表达部分逆转了mir -511-3p诱导的MASLD抑制。此外，ROCK2的敲除可以减轻norad引起的MASLD恶化。此外，过表达NORAD或ROCK2或干扰miR-511-3p会影响resmetin治疗抑制MASLD的发展。最后，由NORAD/miR-511-3p/Rock2轴和NORAD/ Rock2相互作用驱动的肝脏代谢变化也影响白色脂肪生长、胰腺β细胞去分化和肝纤维化。结论：NORAD/miR-511-3p/Rock2轴和NORAD/ Rock2相互作用在MASLD进展中发挥关键作用，确定其治疗的潜在治疗靶点。

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

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

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