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KMID : 0880220230610070693
Journal of Microbiology
2023 Volume.61 No. 7 p.693 ~ p.702
Fibroblast Growth Factor 11 Inhibits Hepatitis B Virus Gene Expression Through FXR¥á Suppression
Seong Mi-So

Jang Jeong-Ah
Jeong Ye-Rim
Kim Ye-Bin
Yi Yi Kyaw
Kong Hee-Jeong
Lee Jung-Hyun
Cheong Jae-Hun
Abstract
Fibroblast growth factor 11 (FGF11) is a member of the intracellular FGF family, which shows different signal transmission compared with other FGF superfamily members. The molecular function of FGF11 is not clearly understood. In this study, we identified the inhibitory effect of FGF11 on hepatitis B virus (HBV) gene expression through transcriptional suppression. FGF11 decreased the mRNA and protein expression of HBV genes in liver cells. While the nuclear receptor FXR¥á1 increased HBV promoter transactivation, FGF11 decreased the FXR¥á-mediated gene induction of the HBV promoter by the FXR¥á agonist. Reduced endogenous levels of FXR¥á by siRNA and the dominant negative mutant protein (aa 1?187 without ligand binding domain) of FXR¥á expression indicated that HBV gene suppression by FGF11 is dependent on FXR¥á inhibition. In addition, FGF11 interacts with FXR¥á protein and reduces FXR¥á protein stability. These results indicate that FGF11 inhibits HBV replicative expression through the liver cell-specific transcription factor, FXR¥á, and suppresses HBV promoter activity. Our findings may contribute to the establishment of better regimens for the treatment of chronic HBV infections by including FGF11 to alter the bile acid mediated FXR pathway.
KEYWORD
FGF11, Hepatitis B virus, HBx protein, FXR, Antiviral effect
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