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Download Treatment with Peg-Interferon α-2b for HBeAg
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Treatment with Peg-Interferon α-2b for HBeAg-Positive Chronic Hepatitis B : HBsAg Loss Is Associated with HBV Genotype Hajo J. Flink, M.Sc.,1 Monika van Zonneveld, M.D., Ph.D., Bettina E. Hansen, M.Sc., Robert A. de Man, M.D., Ph.D., Solko W. Schalm, M.D., Ph.D., Harry L.A. Janssen, M.D., Ph.D., for the HBV 99-01 Study Group Am J Gastroenterol 2006;101:297–303 INTRODUCTION • Chronic HBV infection :defined as HBsAg positivity for > 6 mo. ass. with risk ↑ of developing cirrhosis, hepatic decompensation, hepatocellular carcinoma • Loss of HBsAg : improved long-term outcome risk ↓ of hepatic decompensation & hepatocellular carcinoma • Purpose of therapy for chr. hepatitis B is serum HBsAg negativity. INTRODUCTION • nucleoside or nucleotide analogues : reactivation after Tx termination HBV variants in continuous Tx • lamivudine : < 2% loss of HBsAg adefovir dipivoxil : 1.6% loss of HBsAg INTRODUCTION : Tx with PEG INF α-2b is effective for HBeAg(+) HBV. Combination with lamivudine not superior to monotherapy. →to investigate incidence of & factors predicting HBsAg loss due to treatment with Peg-IFN α-2b alone or with lamivudine PATIENTS • 266 pt were analyzed • Inclusion : >16 yr (+) for HBsAg & HBeAg for > 6 mo. elevated ALT levels (2 time ULN) • Exclusion : antiviral or immune modulatory treatment anti-HCV,HDV,HIV Ab , pregnancy decompensated liver disease drug or alcohol abuse, HCC inadequate hematological levels serum AFP > 50 ng/mL hypo-,hyperthyroidism, contraIx for IFN α. Study Design 100 ug/wk Peg-IFN α-2b for 32 wk with placebo 50 ug/wk Peg-IFN α2b ,32~52 wk with placebo Post F/U 26wks 100 ug/wk Peg-IFN α-2b for 32wk with Lamivudine 100mg 50 ug/wk Peg-IFN α2b ,32~52wk with Lamibudine 100 mg RESULTS Figure 1. Course of serum HBeAg, HBsAg, and PCRnegativity (<400 copies/mL) during Tx & F/U. Table 1. Pt Data on Nonresponders, HBeAg Responders, HBsAg Responders Figure 2. HBV DNA response & ALT normalization at end of F/U in HBeAg(+) HBeAg(-), HBsAg(-) pt at the end of F/U. Table 2. Baseline Characteristics and Geographical Distribution of pt with HBV Genotype A, B, C, D Figure 3. Proportion of HBeAg and HBsAg clearance at end of F/U according to genotype Genotype A versus D (p=0.006) CONCLUSIONS • Peg-IFN α-2b for HBeAg-positive pt led to HBsAg loss in 7% , higher than for lamivudine or adefovir . • treatment with Peg-IFN α-2b , best therapy to achieve HBsAg clearance in pt with genotype A.
