Your search keyword '"Mihm, U."' showing total 8 results

1. Hepatitis C viral dynamics during ribavirin priming differ according to prior treatment response and HCV type.

Author

Fülöp, B., Mihm, U., Rohde, P., Buggisch, P., Schlosser, B., Biermer, M., Brodzinski, A., Fischer, J., Böhm, S., Bömmel, F., Sarrazin, C., and Berg, T.

Subjects

*HEPATITIS C treatment, *RIBAVIRIN, *ANTIVIRAL agents, *DRUG efficacy, *MEDICAL virology, *COMBINATION drug therapy

Abstract

The mode of action of ribavirin is not completely understood. Ribavirin monotherapy has a measurable antiviral effect, which shows great variability. It might lead to an earlier steady state of plasma concentration and therefore enhance the effect of following combination treatment. The aim of this study was to evaluate the antiviral effect of ribavirin priming and its influence on sustained virologic response after combination treatment in a group of patients with different hepatitis C virus ( HCV) types with or without prior treatment experience. Retrospective analysis of 75 patients (37 treatment naïve, 20 prior relapse, 16 prior nonresponse, genotype 1 present in 60 patients) from five centres who received ribavirin priming as part of an individual strategy in order to improve treatment outcome. All patients received ribavirin monotherapy with a mean dose of 14.5 mg kg−1 body weight for a mean of 28 days. After ribavirin priming, dual combination treatment with pegylated interferon alfa and ribavirin was started. The mean HCV RNA decline after ribavirin priming was 0.6 log10 IU mL−1 ( P<.001). The initial viral decline depended on HCV type and previous treatment status being highest among prior relapsers (0.8 log10 IU mL−1; P=.002) and HCV type 2/3 (1.2 log10 IU mL−1; P=.05) and lowest among those with prior nonresponse (0.3 log10 IU mL−1, P=.01). IFNL4 (formerly IL28B) genotype for rs12979860 and IFNL3 genotype rs8099917 did not influence the initial viral decline. The study demonstrates a significant variability in the viral dynamics and antiviral efficacy of ribavirin monotherapy, which is mainly influenced by prior treatment status. The fact that the lowest response pattern was observed in prior nonresponder patients to pegylated interferon alfa plus ribavirin combination therapy can be taken as a hint that not only the individual interferon, but also the ribavirin sensitivity contributes significantly to the nonresponsive state. [ABSTRACT FROM AUTHOR]

Published

2016

2. Impact of ribavirin priming on viral kinetics and treatment response in chronic hepatitis C genotype 1 infection.

Author

Mihm, U., Welker, M.‐W., Teuber, G., Wedemeyer, H., Berg, T., Sarrazin, C., Böhm, S., Alshuth, U., Herrmann, E., and Zeuzem, S.

Subjects

*RIBAVIRIN, *HEPATITIS C, *VIRAL disease treatment, *CELLULAR signal transduction, *POLYETHYLENE glycol, *PLACEBOS, *BODY weight

Abstract

Ribavirin amplifies the interferon-alpha (IFN) signalling cascade. As ribavirin needs 4 weeks to reach steady state, ribavirin priming may optimize hepatic IFN sensitivity before starting a pegylated (PEG)-IFN/ribavirin combination therapy. This study investigated potential benefits of ribavirin priming prior to PEG-IFN2a/ribavirin combination therapy on viral kinetics, on-treatment and sustained virological response (SVR) in chronic hepatitis C virus (HCV) genotype 1 infection. Sixty-eight treatment naive patients were randomized 2:2:1 to ribavirin (ribavirin arm) or placebo (placebo arm) or PEG-IFN2a (PEG-IFN2a arm) for 6 weeks prior to 12 weeks of PEG-IFN2a/ribavirin combination therapy within a double-blind, placebo-controlled trial. Then, standard PEG-IFN2a/ribavirin combination therapy according to the German guidelines was continued under the responsibility of the investigators. Ribavirin was given according to body weight and PEG-IFN2a at a dose of 180 μg subcutaneously once/week. During ribavirin priming, HCV RNA showed a decline of −0.58 log10 IU/mL ( P < 0.001) that was unrelated to the IL28B rs12979860 genotype (CC vs CT/TT, P = 0.244). Ribavirin priming did neither increase the PEG-IFN2a-induced first- or second-phase viral decline ( P values >0.100) nor on-treatment response or SVR (HCV RNA undetectable at week 12 of combination therapy: ribavirin arm 56%, placebo arm 38%, PEG-IFN2a arm 50%; SVR: ribavirin arm 41%, placebo arm 54%, PEG-IFN2a arm 50%; P values >0.300). In conclusion, ribavirin monotherapy showed a significant antiviral activity that was not influenced by the IL28B genotype. Ribavirin priming prior to PEG-IFN2a/ribavirin combination therapy did neither increase the first- or second-phase viral decline nor on-treatment response or SVR. [ABSTRACT FROM AUTHOR]

Published

2014

3. Effect of ribavirin on the frequency of RNase L cleavage sites within the hepatitis C viral genome.

Author

Mihm, U., Hofmann, W. P., Welsch, C., Polta, A., Lengauer, T., Zeuzem, S., Sarrazin, C., and Herrmann, E.

Subjects

*RIBAVIRIN, *HEPATITIS C virus, *NUCLEOTIDES, *MUTAGENESIS, *GASTROENTEROLOGY, *GUANOSINE triphosphate, *INTERFERONS

Abstract

The mechanisms of synergy in antiviral activity of interferon-α and ribavirin in treating chronic hepatitis C virus (HCV) infection are still unknown. Interferon-α indirectly induces cleavage of viral RNA by RNase L at UU/UA dinucleotides. There is evidence that HCV genomes with a higher number of UU/UA dinucleotides are more sensitive to interferon-α. As a guanosine analogue, ribavirin exerts a mutagenic effect promoting G-to-A and C-to-U transitions. This study investigates whether ribavirin-induced mutagenesis causes a higher frequency of UU/UA dinucleotides in the viral progeny sequences. Increased mutational frequencies in favour of G-to-A and C-to-U transitions during ribavirin treatment was reported by Hofmann et al. (Gastroenterology 2007;132:921–930). Overall, 937 nucleotide sequences from that publication were reanalysed for RNase L cleavage sites. These included HCV NS3 quasispecies from three patients with ribavirin monotherapy and NS5B quasispecies from patients who received ribavirin alone ( n = 7) or in combination with interferon-α ( n = 7) at baseline and during treatment; NS5B quasispecies from a subgenomic HCV replicon system after 24, 48 and 72 h of cultivation with or without ribavirin or with levovirin. For NS3 quasispecies during ribavirin monotherapy and NS5B quasispecies from patients who received ribavirin alone or in combination with interferon-α, analysis of RNase L cleavage sites did not reveal changes during treatment or differences between treatment regimes. Similarly, RNaseL cleavage sites from NS5B quasispecies of the HCV replicon did not differ significantly between time points or treatments. In conclusion, Ribavirin-induced mutagenesis did not increase RNase L cleavage sites (UU/UA dinucleotides) within the HCV NS3 or NS5B encoding regions. [ABSTRACT FROM AUTHOR]

Published

2010

4. Prospective study of bone mineral density and metabolism in patients with chronic hepatitis C during pegylated interferon α and ribavirin therapy.

Author

Hofmann, W. P., Kronenberger, B., Bojunga, J., Stamm, B., Herrmann, E., Bücker, A., Mihm, U., von Wagner, M., Zeuzem, S., and Sarrazin, C.

Subjects

OSTEOPOROSIS, LIVER diseases, METABOLISM, BONE diseases, THERAPEUTICS

Abstract

The importance of osteoporosis as a complication of end-stage liver disease is well known. However, significant osteopenia may occur in earlier stages of chronic hepatitis C (CHC). Furthermore, antiviral therapy may influence bone metabolism. Thirty patients with CHC genotype 1 infection and without established cirrhosis were treated with peginterferon-alfa and ribavirin. Dual-energy x-ray absorptiometry was performed at baseline, after 48 weeks of therapy, and by the end of a 24-week follow-up period. Bone mineral density (BMD), T-scores, and Z-scores were assessed. Serum C-terminal propeptide of type I collagen (CICP) and osteocalcin levels were measured. Thirteen patients had osteopenia (43%) and osteoporosis was present in four patients (13%). Antiviral therapy led to significant on-treatment increases of lumbar spine and hip BMD ( P ≤ 0.05) as well as T-scores ( P ≤ 0.05) and Z-scores ( P ≤ 0.01) irrespective of subsequent treatment response. Further analyses showed that in patients with sustained virological response ( n = 19) most parameters remained highly above baseline values by the end of the 24-week follow-up period, while patients with virological relapse ( n = 11) had decreases of BMD, T-scores and Z-scores thereafter that did not differ from baseline. Serum CICP and osteocalcin levels decreased during therapy. Osteocalcin levels remained below baseline in sustained responder, but showed an increase in relapsers by the end of the 24-week follow-up ( P ≤ 0.05). Osteopenia is detectable in a substantial proportion of CHC patients without established cirrhosis. Antiviral therapy leads to an on-treatment increase of BMD, which may last in those patients who achieve a sustained virological response. [ABSTRACT FROM AUTHOR]

Published

2008

5. Somatic hypermutation and mRNA expression levels of the BCL-6 gene in patients with hepatitis C virus-associated lymphoproliferative diseases.

Author

Hofmann, W. P., Fernandez, B., Herrmann, E., Welsch, C., Mihm, U., Kronenberger, B., Feldmann, G., Spengler, U., Zeuzem, S., and Sarrazin, C.

Subjects

MESSENGER RNA, GENES, HEPATITIS C virus, LYMPHOPROLIFERATIVE disorders, CRYOGLOBULINEMIA, ONCOGENES

Abstract

Chronic hepatitis C virus (HCV) infection leads to mixed cryoglobulinaemia (MC) and B-cell non-Hodgkin lymphoma (B-NHL). Aberrant somatic hypermutation and deregulation of the oncogene BCL-6 is associated with lymphomagenesis. Recently, HCV was shown to induce BCL-6 mutations in vitro. The BCL-6 gene (area B) was cloned and sequenced from peripheral blood mononuclear cells (PBMC) of 21 chronically HCV-infected patients with or without MC and B-NHL, and six healthy controls. Mutational frequencies, genetic complexity and diversity were calculated. BCL-6 mRNA from PBMC was quantified by real-time polymerase chain reaction, and additional sustained virologic responders to antiviral therapy and HBV patients served as controls. The overall/recurrent mutational frequencies tended to be lower in MC and B-NHL patients when compared with controls ( P = 0.15 and 0.06, respectively). Genetic complexity was significantly lower in MC and B-NHL patients ( P = 0.025). BCL-6 mRNA concentration was decreased in all HCV patients when compared with healthy controls, sustained virologic responder and HBV patients ( P = 0.005). Although HCV can induce BCL-6 mutations in vitro, lower mutational frequencies and decreased BCL-6 mRNA expression in vivo suggest no major role of aberrant somatic hypermutation in HCV-associated MC and B-NHL. [ABSTRACT FROM AUTHOR]

Published

2007

6. Review article: predicting response in hepatitis C virus therapy.

Author

MIHM, U., HERRMANN, E., SARRAZIN, C., and ZEUZEM, S.

Subjects

*RIBAVIRIN, *INTERFERONS, *HEPATITIS C, *ANTIVIRAL agents, *CIRRHOSIS of the liver, *HEPATITIS C virus

Abstract

The introduction of combination therapy with ribavirin and of pegylated interferons has improved treatment results in patients with chronic hepatitis C. However, overall rates of sustained virologic response following antiviral therapy of chronic hepatitis C still do not exceed 54–63%. Because of several virus- and patient-related factors, treatment is even less successful in some patient subpopulations. The major viral factors associated with impaired response are hepatitis C virus genotype 1 infection and a high viral load. Among patient-related factors cirrhosis is of special importance. Baseline predictive factors for sustained virologic response become less important for prediction of treatment outcome when quantifications of hepatitis C virus RNA during early therapy are taken into account. This article provides a summary of virus- and patient-related parameters, which are prognostic for response to antiviral therapy in chronic hepatitis C and focuses on the prediction of treatment response by quantification of hepatitis C virus RNA concentration during therapy. [ABSTRACT FROM AUTHOR]

Published

2006

7. Apoptotic cytokeratin 18 neoepitopes in serum of patients with chronic hepatitis C.

Author

Kronenberger, B., Wagner, M., Herrmann, E., Mihm, U., Piiper, A., Sarrazin, C., and Zeuzem, S.

Subjects

HEPATITIS C, AMINOTRANSFERASES, APOPTOSIS, VIRAL hepatitis, LIVER diseases, HEPATITIS

Abstract

In patients with chronic hepatitis C, alanine aminotransferase (ALT) levels do not accurately reflect the extent of liver inflammation. The discrepancy between ALT level and liver damage could be related to the mode of cell death. In the present study, we quantified serum levels of apoptotic cytokeratin 18 (CK-18) neoepitopes that are generated by activated caspases during apoptosis. Apoptotic CK-18 neoepitopes were quantified by enzyme linked immunosorbent assay in sera from patients with chronic hepatitis C and elevated ALT levels (n = 72), patients with chronic hepatitis C and persistently normal ALT levels (n = 27) and healthy controls (n = 19). Serum CK-18 neoepitope levels were strongly correlated with ALT (r = 0.659,P < 0.0001) and the histology activity index (r = 0.374,P < 0.001). Patients with chronic hepatitis C and persistently normal ALT levels had higher apoptotic CK-18 neoepitope levels than healthy controls (P = 0.03) but lower levels than patients with chronic hepatitis C and elevated ALT levels (P < 0.001). Highest serum CK-18 neoepitope levels were observed in patients with cirrhosis (P = 0.002). Hence apoptotic CK-18 neoepitopes in serum of patients with chronic hepatitis C are associated with ALT level and histological liver damage. Serum apoptotic CK-18 neoepitope levels are elevated both in patients with chronic hepatitis C and elevated ALT levels as well as in patients with normal ALT levels indicating that also patients with chronic hepatitis C and normal ALT have an increased hepatocyte loss by apoptosis. [ABSTRACT FROM AUTHOR]

Published

2005

8. Optimal therapy in genotype 1 patients.

Author

Farnik H, Mihm U, and Zeuzem S

Subjects

Antiviral Agents pharmacology, Dose-Response Relationship, Drug, Drug Therapy, Combination, Genotype, Hepacivirus drug effects, Humans, Interferon alpha-2, Interferon-alpha pharmacology, Polyethylene Glycols, Recombinant Proteins, Time Factors, Antiviral Agents therapeutic use, Hepacivirus genetics, Hepatitis C drug therapy, Hepatitis C genetics, Interferon-alpha therapeutic use, Ribavirin therapeutic use

Abstract

Most infections with hepatitis C virus (HCV) fail to resolve spontaneously and progress to chronic hepatitis C. Genotype 1 HCV accounts for most hepatitis C infections in North America, Western Europe, and Japan. Patients infected with HCV genotype 1 are the most resistant to treatment, which results in poor treatment outcomes. Although sustained virologic response (SVR) rates have significantly improved with introduction of combination therapy with pegylated interferon alfa and ribavirin, the rates are still lower than those in genotype 2 or 3 infections. This review discusses how treatment outcomes in patients with HCV genotype 1 infection can be optimized by using the drugs currently licensed for treatment of hepatitis C: pegylated interferon alfa-2a/b and ribavirin. Dose modifications and variations of treatment duration are the two strategies that have been investigated best, so far. Treatment--naïve patients and non-responders and relapsers to prior antiviral therapy are discussed separately.

Published

2009