Essential metabolic, anti-inflammatory, and anti-tumorigenic functions of miR-122 in liver
Shu-hao Hsu, … , Joshua T. Mendell, Kalpana Ghoshal
Shu-hao Hsu, … , Joshua T. Mendell, Kalpana Ghoshal
Published July 23, 2012
Citation Information: J Clin Invest. 2012;122(8):2871-2883. https://doi.org/10.1172/JCI63539.
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Research Article

Essential metabolic, anti-inflammatory, and anti-tumorigenic functions of miR-122 in liver

Abstract

miR-122, an abundant liver-specific microRNA (miRNA), regulates cholesterol metabolism and promotes hepatitis C virus (HCV) replication. Reduced miR-122 expression in hepatocellular carcinoma (HCC) correlates with metastasis and poor prognosis. Nevertheless, the consequences of sustained loss of function of miR-122 in vivo have not been determined. Here, we demonstrate that deletion of mouse Mir122 resulted in hepatosteatosis, hepatitis, and the development of tumors resembling HCC. These pathologic manifestations were associated with hyperactivity of oncogenic pathways and hepatic infiltration of inflammatory cells that produce pro-tumorigenic cytokines, including IL-6 and TNF. Moreover, delivery of miR-122 to a MYC-driven mouse model of HCC strongly inhibited tumorigenesis, further supporting the tumor suppressor activity of this miRNA. These findings reveal critical functions for miR-122 in the maintenance of liver homeostasis and have important therapeutic implications, including the potential utility of miR-122 delivery for selected patients with HCC and the need for careful monitoring of patients receiving miR-122 inhibition therapy for HCV.

Authors

Shu-hao Hsu, Bo Wang, Janaiah Kota, Jianhua Yu, Stefan Costinean, Huban Kutay, Lianbo Yu, Shoumei Bai, Krista La Perle, Raghu R. Chivukula, Hsiaoyin Mao, Min Wei, K. Reed Clark, Jerry R. Mendell, Michael A. Caligiuri, Samson T. Jacob, Joshua T. Mendell, Kalpana Ghoshal

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Figure 3

Mir122-LKO and -KO mice develop hepatitis and fibrosis with age.

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Mir122-LKO and -KO mice develop hepatitis and fibrosis with age. (A a...
(A and C) Portal inflammation, steatosis, and fibrosis in 6-month-old LKO (A) and KO (C) mice. The inset in A depicts foci of altered hepatocytes as observed in some livers. Eight to 10 mice of each genotype were analyzed after overnight fasting. Scale bars for A: top row, 200 μm; second and third rows and inset, 25 μm; fourth row, 200 μm. Scale bars for C: top row, 200 μm; middle row, 25 μm; bottom row, 100 μm. (B and D) Inflammation, steatosis, and fibrosis scores generated through blinded evaluation of histopathology. (E) Hepatic TG and cholesterol levels in 6-month-old mice. The results shown in BD are mean ± SD. Statistical significance was calculated using a 2-tailed t test.