Hepatic MIR20B promotes nonalcoholic fatty liver disease by suppressing PPARA

Yo Han Lee; Hyun-Jun Jang; Sounkou Kim; Sun Sil Choi; Keon Woo Khim; Hye-jin Eom; Jimin Hyun; Kyeong Jin Shin; Young Chan Chae; Hongtae Kim; Jiyoung Park; Neung Hwa Park; Chang-Yun Woo; Chung Hwan Hong; Eun Hee Koh; Dougu Nam; Jang Hyun Choi

doi:10.7554/eLife.70472

eLife (Dec 2021)

Hepatic MIR20B promotes nonalcoholic fatty liver disease by suppressing PPARA

Yo Han Lee,
Hyun-Jun Jang,
Sounkou Kim,
Sun Sil Choi,
Keon Woo Khim,
Hye-jin Eom,
Jimin Hyun,
Kyeong Jin Shin,
Young Chan Chae,
Hongtae Kim,
Jiyoung Park,
Neung Hwa Park,
Chang-Yun Woo,
Chung Hwan Hong,
Eun Hee Koh,
Dougu Nam,
Jang Hyun Choi

Affiliations

Yo Han Lee: ORCiD; Department of Biological Sciences, Ulsan National Institute of Science and Technology, Ulsan, Republic of Korea
Hyun-Jun Jang: ORCiD; Department of Biological Sciences, Ulsan National Institute of Science and Technology, Ulsan, Republic of Korea
Sounkou Kim: Department of Biological Sciences, Ulsan National Institute of Science and Technology, Ulsan, Republic of Korea
Sun Sil Choi: Department of Biological Sciences, Ulsan National Institute of Science and Technology, Ulsan, Republic of Korea
Keon Woo Khim: Department of Biological Sciences, Ulsan National Institute of Science and Technology, Ulsan, Republic of Korea
Hye-jin Eom: Department of Biological Sciences, Ulsan National Institute of Science and Technology, Ulsan, Republic of Korea
Jimin Hyun: Department of Biological Sciences, Ulsan National Institute of Science and Technology, Ulsan, Republic of Korea
Kyeong Jin Shin: Department of Biological Sciences, Ulsan National Institute of Science and Technology, Ulsan, Republic of Korea
Young Chan Chae: Department of Biological Sciences, Ulsan National Institute of Science and Technology, Ulsan, Republic of Korea
Hongtae Kim: Department of Biological Sciences, Ulsan National Institute of Science and Technology, Ulsan, Republic of Korea
Jiyoung Park: ORCiD; Department of Biological Sciences, Ulsan National Institute of Science and Technology, Ulsan, Republic of Korea
Neung Hwa Park: Department of Internal Medicine, Ulsan University Hospital, Ulsan, Republic of Korea
Chang-Yun Woo: Department of Internal Medicine, Asan Medical Center, Seoul, Republic of Korea
Chung Hwan Hong: Department of Medical Science, Asan Medical Center, Seoul, Republic of Korea
Eun Hee Koh: Department of Internal Medicine, Asan Medical Center, Seoul, Republic of Korea
Dougu Nam: ORCiD; Department of Biological Sciences, Ulsan National Institute of Science and Technology, Ulsan, Republic of Korea
Jang Hyun Choi: ORCiD; Department of Biological Sciences, Ulsan National Institute of Science and Technology, Ulsan, Republic of Korea

DOI: https://doi.org/10.7554/eLife.70472
Journal volume & issue: Vol. 10

Abstract

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Background: Non-alcoholic fatty liver disease (NAFLD) is characterized by excessive lipid accumulation and imbalances in lipid metabolism in the liver. Although nuclear receptors (NRs) play a crucial role in hepatic lipid metabolism, the underlying mechanisms of NR regulation in NAFLD remain largely unclear. Methods: Using network analysis and RNA-seq to determine the correlation between NRs and microRNA in human NAFLD patients, we revealed that MIR20B specifically targets PPARA. MIR20B mimic and anti-MIR20B were administered to human HepG2 and Huh-7 cells and mouse primary hepatocytes as well as high-fat diet (HFD)- or methionine-deficient diet (MCD)-fed mice to verify the specific function of MIR20B in NAFLD. We tested the inhibition of the therapeutic effect of a PPARα agonist, fenofibrate, by Mir20b and the synergic effect of combination of fenofibrate with anti-Mir20b in NAFLD mouse model. Results: We revealed that MIR20B specifically targets PPARA through miRNA regulatory network analysis of nuclear receptor genes in NAFLD. The expression of MIR20B was upregulated in free fatty acid (FA)-treated hepatocytes and the livers of both obesity-induced mice and NAFLD patients. Overexpression of MIR20B significantly increased hepatic lipid accumulation and triglyceride levels. Furthermore, MIR20B significantly reduced FA oxidation and mitochondrial biogenesis by targeting PPARA. In Mir20b-introduced mice, the effect of fenofibrate to ameliorate hepatic steatosis was significantly suppressed. Finally, inhibition of Mir20b significantly increased FA oxidation and uptake, resulting in improved insulin sensitivity and a decrease in NAFLD progression. Moreover, combination of fenofibrate and anti-Mir20b exhibited the synergic effect on improvement of NAFLD in MCD-fed mice. Conclusions: Taken together, our results demonstrate that the novel MIR20B targets PPARA, plays a significant role in hepatic lipid metabolism, and present an opportunity for the development of novel therapeutics for NAFLD. Funding: This research was funded by Korea Mouse Phenotyping Project (2016M3A9D5A01952411), the National Research Foundation of Korea (NRF) grant funded by the Korea government (2020R1F1A1061267, 2018R1A5A1024340, NRF-2021R1I1A2041463, 2020R1I1A1A01074940, 2016M3C9A394589324), and the Future-leading Project Research Fund (1.210034.01) of UNIST.

Published in eLife

ISSN: 2050-084X (Online)
Publisher: eLife Sciences Publications Ltd
Country of publisher: United Kingdom
LCC subjects: Medicine; Science: Biology (General)
Website: https://elifesciences.org

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