The results suggested that the alcohol-induced
increase in expression of HSP90 might augment HCV replication by stabilizing selleck miR-122 binding to the HCV genome and/or enhancing GW182 gene expression. We speculate that HSP90 regulation of GW182 expression depends on the chaperone and/or the stabilizing effect of HSP90 and not by direct transcriptional regulation by HSP90 as the GW182 promoter has no consensus binding motif for heat shock elements (NCBI GW182 reference sequences: NM_018996.3 and NM_001142640.1). Additionally, inhibition of HSP90 activity, similar to GW182 inhibition, affected the abundance of miR-122, supporting the hypothesis that HSP90 could promote GW182 expression, which can regulate miR-122 expression. These observations cannot rule out participation of other co-chaperones. Our results, together with previous reports,31, 44 suggest that HSP90 has multiple roles in HCV replication, including direct interaction with CHIR-99021 cell line viral proteins, regulating GW182 gene expression, and the abundance of miR-122. We demonstrated that HSP90 works as a regulator of miR-122 abundance, because inhibiting HSP90
activity with an inhibitor or with HSP90-specific siRNAs significantly reduced miR-122 expression. These data suggest that ethanol as a cellular stress inducer acts through the stress-responsive transcription factor, HSP90, to regulate miR-122 expression. Interestingly, we also found GW182, a GWB component, to affect the expression of miR-122, and future studies may reveal roles of other GWB components in miR-122 abundance or other miRNAs. However, 上海皓元医药股份有限公司 we found that ethanol exposure had no effects on miR-370 (Supporting Fig. 1F) that also modulates miR-122 expression,45 indicating that miR-370 might not be involved in this process. In conclusion, our data suggest that ethanol facilitates
HCV replication involving GW182 and HSP90 modulation. In the context of alcohol abuse, we show for the first time that GW182 and HSP90 are host factors that spur disease progression in HCV infection. Our studies provide experimental evidence for the possible use of GW182 and HSP90 inhibitors as feasible targets to interfere with HCV replication and the undesirable effects of alcohol use in HCV infection. We are grateful to Drs. Charles M. Rice and Takaji Wakita for kindly providing reagents and Dr. Tuschl for the GW182 overexpression plasmid. Additional Supporting Information may be found in the online version of this article. “
“The low-grade inflammatory state present in obesity contributes to obesity-related metabolic dysregulation, including nonalcoholic steatohepatitis (NASH) and insulin resistance. Intercellular interactions between immune cells or between immune cells and hepatic parenchymal cells contribute to the exacerbation of liver inflammation and steatosis in obesity. The costimulatory molecules, B7.1 and B7.