Gene expression profiles associated with depression in patients with chronic hepatitis C ( CH ‐C)

The standard treatment for CH ‐ C , pegylated interferon‐α and ribavirin ( PEG ‐ IFN  +  RBV ), is associated with depression. Recent studies have proposed a new role for cytokines in the pathogenesis of depression. We aimed to assess differential gene expression related to depression in CH ‐ C patients treated with PEG ‐ IFN  +  RBV . We included 67 CH ‐ C patients being treated with PEG ‐ IFN + RBV . Of the entire study cohort, 22% had pre‐existing depression, while another 37% developed new depression in course of the treatment. Pretreatment blood samples were collected into PAXgene ™ RNA tubes, the RNA s extracted from peripheral blood mononuclear cells ( PBMC s) were used for one step RT ‐ PCR to profile 160 m RNA s. Differentially expressed genes were separated into up‐ and down‐regulated genes according to presence or absence of depression at baseline (pre‐existing depression) or following the initiation of treatment (treatment‐related depression). The m RNA expression profile associated with any depression and with treatment‐related depression included four and six genes, respectively. Our data demonstrate a significant down‐regulation of TGF ‐β1 and the shift of Th1‐Th2 cytokine balance in the depression associated with IFN ‐based treatment of HCV infection. We propose that TGF ‐β1 plays an important role in the imbalance of Th1/Th2 in patients with CH ‐ C and depression. With further validation, TGF ‐β1 and other components of Th1/Th2 regulation pathway may provide a future marker for CH ‐ C patients predisposed to depression.