miR-33 deletion in hepatocytes attenuates MASLD-MASH-HCC progression
Pablo Fernández-Tussy, … , Yajaira Suárez, Carlos Fernández-Hernando
Pablo Fernández-Tussy, … , Yajaira Suárez, Carlos Fernández-Hernando
Published August 27, 2024
Citation Information: JCI Insight. 2024;9(19):e168476. https://doi.org/10.1172/jci.insight.168476.
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Research Article Hepatology Metabolism

miR-33 deletion in hepatocytes attenuates MASLD-MASH-HCC progression

Abstract

The complexity of the mechanisms underlying metabolic dysfunction–associated steatotic liver disease (MASLD) progression remains a significant challenge for the development of effective therapeutics. miRNAs have shown great promise as regulators of biological processes and as therapeutic targets for complex diseases. Here, we study the role of hepatic miR-33, an important regulator of lipid metabolism, during the progression of MASLD and the development of hepatocellular carcinoma (HCC). We report that miR-33 was elevated in the livers of humans and mice with MASLD and that its deletion in hepatocytes (miR-33 HKO) improved multiple aspects of the disease, including steatosis and inflammation, limiting the progression to metabolic dysfunction–associated steatotic hepatitis (MASH), fibrosis, and HCC. Mechanistically, hepatic miR-33 deletion reduced lipid synthesis and promoted mitochondrial fatty acid oxidation, reducing lipid burden. Additionally, absence of miR-33 altered the expression of several known miR-33 target genes involved in metabolism and resulted in improved mitochondrial function and reduced oxidative stress. The reduction in lipid accumulation and liver injury resulted in decreased YAP/TAZ pathway activation, which may be involved in the reduced HCC progression in HKO livers. Together, these results suggest suppressing hepatic miR-33 may be an effective therapeutic approach to temper the development of MASLD, MASH, and HCC in obesity.

Authors

Pablo Fernández-Tussy, Magdalena P. Cardelo, Hanming Zhang, Jonathan Sun, Nathan L. Price, Nabil E. Boutagy, Leigh Goedeke, Martí Cadena-Sandoval, Chrysovalantou E. Xirouchaki, Wendy Brown, Xiaoyong Yang, Oscar Pastor-Rojo, Rebecca A. Haeusler, Anton M. Bennett, Tony Tiganis, Yajaira Suárez, Carlos Fernández-Hernando

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Figure 3

miR-33 deficiency in hepatocytes increases FAO synthesis and decreases FA synthesis.

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miR-33 deficiency in hepatocytes increases FAO synthesis and decreases F...
(A) Ex vivo analysis of FAO in WT and HKO livers (n = 5 WT and 4 HKO chow; 6 WT and 6 HKO; MASL; 6 WT and 6 HKO MASH). (B and C) Mitochondrial respiratory analysis inferred from oxygen consumption rate measurements of primary mouse hepatocytes isolated from WT and miR-33 HKO livers (n = 4 WT and 3 HKO MASL; 5 WT and 5 HKO MASH). (D) Western blot and densitometric analysis of CROT, CPT1α, phosphorylated acetyl-CoA carboxylase (p-ACC) (Ser79), total ACC, p-AMPKα (T172), total AMPKα, and housekeeping standard VINCULIN in WT and HKO livers. Data represent the mean ± SEM. *P ≤ 0.05, **P ≤ 0.01, ***P ≤ 0.001 compared with WT animals, unpaired 2-sided Student’s t test for 2-group (B) comparisons and 2-way ANOVA followed by multiple comparison (A and D). CPM, counts per million.