TGF‐β1 mRNA expression in liver biopsy specimens and TGF‐β1 serum levels in patients with chronic hepatitis C before and after antiviral therapy

Summary Background and objective:  Transforming growth factor (TGF)‐ β 1 is the best‐characterized profibrogenic cytokine. TGF‐ β 1 increases the production of extracellular matrix proteins and their receptors and inhibits the synthesis of matrix degrading proteolytic enzymes. We undertook this study to simultaneously evaluate the effect of interferon α 2b plus ribavirin therapy on TGF‐ β 1 daily serum levels and on mRNA TGF‐ β 1 expression in liver biopsy specimens from 60 patients with chronic hepatitis C. Methods:  Serum levels of TGF‐ β 1 were measured by ELISA. The levels of the RNAs in liver biopsy specimens were measured by quantitative reverse transcriptase polymerase chain reaction. After treatment, patients were divided into two groups: 34 responders [undetectable hepatitis C virus (HCV)‐RNA, normal ALT levels, decrease in histology activity index compared with pretreatment liver biposy] and 26 non‐responders (detectable HCV‐RNA, elevated ALT levels, no decrease in the histology activity index). Results and discussion:  In patients with hepatitis C, the ‘responders’ to the antiviral treatment showed significant decreases in both mean daily serum TGF‐ β 1 levels and mRNA TGF‐ β 1 expression in the liver biopsy specimens. The ‘non‐responders’ serum TGF‐ β 1 concentrations did not change significantly, but the mRNA TGF‐ β 1 expression did. Conclusion:  Both serum TGF‐ β 1 concentration and mRNA TGF‐beta1 expression in liver biopsy specimens may be useful as prognostic markers in patients with hepatitis C undergoing antiviral therapy.