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Curcumin Inhibits Hepatitis B Virus Via Down-regulation of the Metabolic Coactivator PGC-1alpha

Overview
Journal FEBS Lett
Specialty Biochemistry
Date 2010 May 4
PMID 20434445
Citations 45
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Abstract

Hepatitis B virus (HBV) infects the liver and uses its cell host for gene expression and propagation. Therefore, targeting host factors essential for HBV gene expression is a potential anti-viral strategy. Here we show that treating HBV expressing cells with the natural phenolic compound curcumin inhibits HBV gene expression and replication. This inhibition is mediated via down-regulation of PGC-1alpha, a starvation-induced protein that initiates the gluconeogenesis cascade and that has been shown to robustly coactivate HBV transcription. We suggest curcumin as a host targeted therapy for HBV infection that may complement current virus-specific therapies.

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