Your search keyword '"Sarrazin, C."' showing total 104 results

1. A phenotypic NS3-protease inhibitor resistance assay to characterize resistance-associated mutations in patients

Author

Rupp, D., Dietz, J., Sikorski, M. A., Sierra, S., Brown, R., Pietschmann, T., Kaiser, R., Sarrazin, C., Bartenschlager, R., Rupp, D., Dietz, J., Sikorski, M. A., Sierra, S., Brown, R., Pietschmann, T., Kaiser, R., Sarrazin, C., and Bartenschlager, R.

Published

2015

2. Impact of HBV genotype and mutations on HBV DNA and qHBsAg levels in patients with HBeAg‐negative chronic HBV infection.

Author

Kuhnhenn, L., Jiang, B., Kubesch, A., Vermehren, J., Knop, V., Susser, S., Dietz, J., Carra, G., Finkelmeier, F., Grammatikos, G., Zeuzem, S., Sarrazin, C., Hildt, E., and Peiffer, K.‐H.

Subjects

HEPATITIS B virus, MOLECULAR microbiology, GENOMES, CELL culture, MEDICAL microbiology

Abstract

Summary: Background: HBV DNA and quantitative (q)HBsAg levels as prognostic markers for HBV‐related disease are mostly validated in Asia and their significance in Western populations is uncertain. Aim: To analyse the impact of the HBV genotype and frequent mutations in precore (PC), basal core promoter (BCP) and preS on HBV DNA and qHBsAg levels. Methods: HBV DNA and qHBsAg serum levels of 465 patients with HBeAg‐negative chronic HBV infection were correlated with the HBV genotype and mutations in PC, BCP and preS. For a detailed analysis of the molecular virology, genotype A2 genomes harbouring these mutations were analysed for replication efficacy and HBsAg release in cell culture. Results: While no impact of the HBV genotype on HBV DNA levels was observed, qHBsAg levels differed up to 1.4 log among the genotypes (P < 0.001), reflected by large differences regarding the 1000 IU/mL HBsAg cut‐off. While PC mutations were associated with higher (P < 0.001), BCP mutations were associated with lower HBV DNA levels (P < 0.001). Higher qHBsAg levels were associated with preS and lower levels with PC mutations (P < 0.001 and P = 0.001, respectively). The cell culture experiments revealed a higher HBsAg release and shorter filaments in case of a HBV genome harbouring a preS deletion. In contrast, a perinuclear HBsAg accumulation was detected for the PC and BCP‐variants, reflecting an impaired HBsAg release. Conclusions: qHBsAg serum levels depend on the HBV genotype and together with HBV DNA levels on frequent mutations in PC, BCP and preS in HBeAg‐negative patients. qHBsAg cut‐offs when used as prognostic markers require genotype‐dependent validation. [ABSTRACT FROM AUTHOR]

Published

2018

3. High efficacy of sofosbuvir/velpatasvir and impact of baseline resistance‐associated substitutions in hepatitis C genotype 3 infection.

Author

von Felden, J., Vermehren, J., Ingiliz, P., Mauss, S., Lutz, T., Simon, K. G., Busch, H. W., Baumgarten, A., Schewe, K., Hueppe, D., Boesecke, C., Rockstroh, J. K., Daeumer, M., Luebke, N., Timm, J., Schulze zur Wiesch, J., Sarrazin, C., and Christensen, S.

Subjects

HEPATITIS C treatment, SOFOSBUVIR, DRUG efficacy, VIRAL nonstructural proteins, INTERFERONS

Abstract

Summary: Background: Twelve weeks of the pangenotypic direct‐acting antiviral (DAA) combination sofosbuvir/velpatasvir (SOF/VEL) was highly efficient in patients with hepatitis C virus (HCV) genotype 3 (GT3) infection in the ASTRAL‐3 approval study. However, presence of resistance‐associated substitutions (RASs) in the HCV nonstructural protein 5A (NS5A) was associated with lower treatment response. Aim: To assess the efficacy and safety of SOF/VEL ± ribavirin (RBV) and the impact of NS5A RASs and RBV use on treatment outcome in HCV GT3 infection in a real‐world setting. Methods: In this multicentre cohort study, GT3 patients from ten treatment centres across Germany were included. Sustained virological response was assessed 12 weeks after end‐of‐treatment (SVR12) in modified intention‐to‐treat (mITT) and per‐protocol analysis (PP). NS5A RASs were tested by population‐based sequencing. Results: A total of 293 GT3 patients were included. The median age was 48 years, 70% were male, 25.3% were cirrhotic, 9.2% were HCV/HIV co‐infected and 21.8% were treatment‐experienced, including 4.1% with DAA experience. Baseline NS5A RASs (Y93H, A30K, L31M) were detected in 11.2%. RBV was added in 5% of noncirrhotic and 58.9% of cirrhotic patients, respectively. SVR12 rates for SOF/VEL±RBV were 95.9% (mITT) and 99.5% (PP), respectively. Only 1 virological relapse occurred in a cirrhotic patient previously treated with SOF/RBV. No treatment‐related major adverse events occurred. Conclusion: Twelve weeks of SOL/VEL±RBV was safe and highly efficient in HCV GT3 across a diverse patient population. Baseline NS5A RASs were rarely observed and presence did not seem to impact SVR, regardless of the use of RBV. [ABSTRACT FROM AUTHOR]

Published

2018

4. Real-world experience with the all-oral, interferon-free regimen of ombitasvir/paritaprevir/ritonavir and dasabuvir for the treatment of chronic hepatitis C virus infection in the German Hepatitis C Registry.

Author

Welzel, T. M., Hinrichsen, H., Sarrazin, C., Buggisch, P., Baumgarten, A., Christensen, S., Berg, T., Mauss, S., Teuber, G., Stein, K., Deterding, K., Bömmel, F., Heyne, R., John, C., Zimmermann, T., Lutz, T., Schott, E., Hettinger, J., Kleine, H., and König, B.

Subjects

RITONAVIR, HEPATITIS C virus, HEPATITIS C treatment, DRUG efficacy, MEDICATION safety, CLINICAL trials

Abstract

Real-world studies are relevant to complement clinical trials on novel antiviral therapies against chronic hepatitis C; however, clinical practice data are currently limited. This study investigated effectiveness and safety of ombitasvir/paritaprevir/ritonavir ( OBV/ PTV/r)±dasabuvir ( DSV)±ribavirin ( RBV) for treatment of HCV genotype ( GT) 1 and GT4 infection in a large real-world cohort. The German Hepatitis C Registry is an observational cohort study prospectively collecting clinical practice data on direct-acting antiviral therapies. Patients with GT1/4 infection treated with OBV/ PTV/r± DSV± RBV were analysed. Effectiveness was assessed by sustained virologic response in 558 patients who reached post-treatment week 12 ( SVR12). Safety is reported in 1017 patients who initiated treatment. Of the patients, 892 (88%) had GT1 and 125 (12%) had GT4 infection. Prior treatment experience and cirrhosis were reported in 598 (59%) and 228 (22%) patients, respectively. Overall, SVR12 ( mITT) was 96% (486/505) in GT1- and 100% (53/53) in GT4 patients. SVR12 rates were high across subgroups including patients with cirrhosis (95%, 123/129), patients with moderate to severe renal impairment (100%, 34/34), and subgroups excluded from registrational trials like patients ≥70 years (96%, 64/67) and failures to prior protease inhibitor treatment (96%, 46/48). Adverse events (AEs) and serious AEs were reported in 52% (525/1017) and 2% (21/1017) of patients, respectively, and led to treatment discontinuation in 1.5% (15/1017) of patients. OBV/ PTV/r± DSV± RBV was effective and generally well tolerated for treatment of HCV infection in clinical practice. [ABSTRACT FROM AUTHOR]

Published

2017

5. No evidence of hepatitis B virus reactivation in patients with resolved infection treated with direct-acting antivirals for hepatitis C in a large real-world cohort.

Author

Mücke, V. T., Mücke, M. M., Peiffer, K.‐H., Weiler, N., Welzel, T. M., Sarrazin, C., Zeuzem, S., Berger, A., and Vermehren, J.

Subjects

VIRUS reactivation, HEPATITIS C treatment, HEPATITIS B treatment, ANTIVIRAL agents, THERAPEUTIC use of interferons, HEPATITIS associated antigen, ALANINE aminotransferase, COMBINATION drug therapy

Abstract

Background Hepatitis B virus ( HBV) reactivation has been observed following interferon ( IFN)-based treatment in HBV/hepatitis C virus ( HCV) co-infected patients. Recent reports suggest that reactivation may also occur in both hepatitis B surface antigen ( HBsAg)-positive and HBsAg-negative patients during HCV treatment with direct-acting antivirals ( DAAs). Aim To investigate the rate of patients with HBV reactivation during IFN-based and IFN-free HCV treatment in a large real-world cohort. Methods A total of 848 patients with chronic hepatitis C were treated with different combinations of DAAs. Among patients with available outcome and HBV data, there were 272 patients hepatitis B core antibody ( HBcAb)-positive ( HBsAg-positive, n=9; HBsAg-negative, n=263), and 536 were HBcAb-negative. All HBcAb-positive patients were tested for HBV DNA at the end of DAA therapy and alanine transaminase ( ALT) levels were frequently measured during therapy and follow-up. Results Seventy-three percent (n=192/263) of HBsAg-negative/ HBcAb-positive patients had elevated ALT levels at baseline, which declined to normal values in all but 18 patients, and no HBV reactivation was observed. Eight patients had detectable but not quantifiable HBV DNA (<20 IU/ mL) at end of treatment, but none were associated with elevated ALT. Five of nine HBsAg-positive/ HBcAb-positive patients experienced transient or permanent HBV reactivation, three of whom required nucleos(t)ide treatment during (n=1) or after (n=2) DAA therapy. Conclusions HBV reactivation was not observed in HBsAg-negative/ HBcAb-positive patients but common in HBsAg-positive/ HBcAb-positive patients treated with different combinations of DAAs for HCV. [ABSTRACT FROM AUTHOR]

Published

2017

6. Real-world use, effectiveness and safety of anti-viral treatment in chronic hepatitis C genotype 3 infection.

Author

Cornberg, M., Petersen, J., Schober, A., Mauss, S., Böker, K. H. W., Link, R., Günther, R., Serfert, Y., Pfeiffer-Vornkahl, H., Manns, M. P., Sarrazin, C., Hüppe, D., Berg, T., and Niederau, C.

Subjects

CHRONIC hepatitis C, CHRONIC diseases, GENOTYPES, ANTIVIRAL agents, DRUG efficacy, THERAPEUTICS

Abstract

Background Treatment of chronic hepatitis C genotype 3 ( GT3) is more challenging compared with other genotypes. Since 2014, several new treatment regimens have been approved but sometimes based on limited data. Aim To validate the use, effectiveness and safety of anti-viral treatment in chronic hepatitis C genotype 3 infection under real-word conditions. Methods The German Hepatitis C-Registry is a large national non-interventional real-world study for patients with chronic hepatitis C. A total of 1322 GT3 patients were enrolled (211 untreated and 1111 treated patients). Results Between February 2014 and September 2015, five different treatment strategies have been used (Peg IFN+ RBV, Peg IFN+ RBV+ SOF, SOF+ RBV, DCV+ SOF± RBV, LDV/ SOF± RBV). Treatment uptake and use of treatment concepts changed markedly and rapidly during the study influenced by new approvals, guideline recommendations, and label updates. Peg IFN-based therapies constantly declined while DCV-based therapies increased with one interruption after the approval of LDV/ SOF, which was frequently used until new guidelines recommended not using this combination for GT3. Per-protocol SVR ranged from 80.9% in the Peg IFN+ RBV group to 96.1% in Peg IFN+ RBV+ SOF treated patients. Treatment-experienced patients with cirrhosis showed a suboptimal SVR of 68% for SOF+ RBV but a high SVR of 90-95% for DCV+ SOF± RBV. The safety analysis showed more adverse events and a stronger decline of haemoglobin for RBV containing regimens. Conclusions Real-world data can validate the effectiveness and safety for treatment regimens that had previously been approved with limited data, in particular for specific subgroups of patients. The present study demonstrates how rapid new scientific data, new treatment guidelines, new drug approvals and label changes are implemented into routine clinical practice today. [ABSTRACT FROM AUTHOR]

Published

2017

7. Regression of fibrosis and portal hypertension in HCV-associated cirrhosis and sustained virologic response after interferon-free antiviral therapy.

Author

Knop, V., Hoppe, D., Welzel, T., Vermehren, J., Herrmann, E., Vermehren, A., Friedrich‐Rust, M., Sarrazin, C., Zeuzem, S., and Welker, M.‐W.

Subjects

HEPATITIS C treatment, PORTAL hypertension, FIBROSIS, ANTIVIRAL agents, CIRRHOSIS of the liver, VIROLOGY

Abstract

It is still controversial, whether and to what amount cirrhosis and portal hypertension are reversible in patients with hepatitis C virus ( HCV)-associated cirrhosis and sustained virologic response ( SVR) after interferon-free antiviral therapy. In this study, we prospectively evaluated dynamics of liver and spleen stiffness in HCV-infected patients with advanced liver disease and SVR after interferon-free treatment. A total of 54 patients with HCV-associated cirrhosis and SVR were included. Liver and spleen stiffness was measured at therapy baseline ( BL), end of treatment ( EOT) and 24 weeks after EOT ( FU24) by transient liver elastography (L- TE) as well as by acoustic radiation force impulse of the liver (L- ARFI) and spleen (S- ARFI), as well as biochemical, virologic and clinical data. Improvement of liver and spleen stiffness was found in 44 of 50 (88%), 31 of 54 (57%) and 25 of 54 (46%) of patients assessed by L- TE, L- ARFI and S- ARFI between baseline and FU24. Liver stiffness assessed by L- TE improved between BL [median (range), 32.5 (9.1-75) kPa] and EOT [median (range), 21.3 (6.7-73.5) kPa; ( P<.0001)], and between BL and FU24 [median (range), 21.2 (5.4-70) kPa; ( P<.0001)]. Liver stiffness assessed by L- ARFI improved between BL [median (range), 2.7 (1.2-4.1) m/s] and FU24 [median (range), 2.4 (1.2-3.9) m/s; P=.002), while spleen stiffness remained unchanged. Our data suggest that improvement of liver stiffness may be rather due to reduced necroinflammation and may be due to a less extent to regression of cirrhosis, as dynamics of liver stiffness improvement was more pronounced between BL and EOT than BL and FU24. [ABSTRACT FROM AUTHOR]

Published

2016

8. 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

9. The efficacy and safety of direct acting antiviral treatment and clinical significance of drug-drug interactions in elderly patients with chronic hepatitis C virus infection.

Author

Vermehren, J., Peiffer, K.‐H., Welsch, C., Grammatikos, G., Welker, M.‐W., Weiler, N., Zeuzem, S., Welzel, T. M., and Sarrazin, C.

Subjects

ANTIVIRAL agents, DRUG efficacy, MEDICATION safety, CHRONIC hepatitis C, DRUG interactions, OLDER patients, INTERFERONS, DISEASES, THERAPEUTICS

Abstract

Background Direct antiviral therapies for chronic hepatitis C virus ( HCV) infection have expanded treatment options for neglected patient populations, including elderly patients who are ineligible/intolerant to receive interferon ( IFN)-based therapy. Aim To investigate the efficacy, tolerability and potential for drug-drug interactions ( DDIs) of IFN-free treatment in patients aged ≥65 years in a large real-world cohort. Methods A total of 541 patients were treated with different combinations of direct antiviral agents ( DAAs: ledipasvir/sofosbuvir ±ribavirin; daclatasvir/sofosbuvir ±ribavirin; paritaprevir/ombitasvir ±dasabuvir ±ribavirin or simeprevir/sofosbuvir ±ribavirin in genotype 1/4, and daclatasvir/sofosbuvir ±ribavirin or sofosbuvir/ribavirin in genotype 2/3). Efficacy, safety and potential DDIs were analysed and compared between patients aged <65 years ( n = 404) and patients aged ≥65 years ( n = 137) of whom 41 patients were ≥75 years. Results Sustained virological response rates were 98% and 91% in patients aged ≥65 years and <65 years, respectively. Elderly patients took significantly more concomitant medications (79% vs. 51%; P < 0.0001). The number of concomitant drugs per patient was highest in patients ≥65 years with cirrhosis (median, three per patient; range, 0-10). Based on the hep-druginteractions database, the proportion of predicted clinically significant DDIs was significantly higher in elderly patients (54% vs. 28%; P < 0.0001). The number of patients who experienced treatment-associated adverse events was similar between the two age groups (63% vs. 65%; P = n.s.). Conclusions Elderly patients are at increased risk for significant DDIs when treated with DAAs for chronic HCV infection. However, with careful pre-treatment assessment of concomitant medications, on-treatment monitoring or dose-modifications, significant DDIs and associated adverse events can be avoided. [ABSTRACT FROM AUTHOR]

Published

2016

10. The macrophage activation marker CD163 is associated with IL28B genotype and hepatic inflammation in chronic hepatitis C virus infected patients.

Author

Dultz, G., Gerber, L., Zeuzem, S., Sarrazin, C., and Waidmann, O.

Subjects

CHRONIC hepatitis C, MACROPHAGE activation, BIOMARKERS, CD antigens, GENOTYPES, INTERLEUKINS, PATIENTS, THERAPEUTICS

Abstract

Recent data highlighted the association of the macrophage activation marker CD163 with histological inflammation and fibrosis in chronic hepatitis C virus ( HCV) infection. The aim of this study was to investigate the influence of successful antiviral treatment and IL28B genotypes on macrophage activation reflected by CD163 levels in HCV infected patients. In a retrospective cohort study, serum sCD163 levels were correlated with results of liver histopathology, IL28B genotyping and clinical parameters in 329 patients with HCV infection, 15 healthy controls and in 161 patients who achieved a sustained virologic response after antiviral treatment. sCD163 levels were significantly higher in patients with chronic HCV infection in comparison to healthy controls (5202 vs 896 ng/mL, P < 0.001). In the multivariate logistic regression analyses, sCD163 was independently associated with histologically determined inflammation ( P = 0.043) but not with fibrosis ( P = 0.091). sCD163 dropped significantly after successful antiviral treatment in comparison to baseline values (5202 vs 3093 ng/mL, P < 0.001). In the univariate analyses, sCD163 was significantly associated with IL28B genotype (C/C vs C/T+T/T) with higher values in the C/C group (6098 vs 4812 ng/mL, P = 0.003). In the multivariate logistic regression model, sCD163 levels were significantly associated with IL28B genotype ( P = 0.003) and sustained virologic response ( SVR) ( P < 0.001). Our data support the association of activated liver macrophages with hepatic necroinflammation in chronic HCV infection as sCD163 levels drop rapidly after SVR. The irresponsiveness of IL28B minor genotypes to interferon might be related to a lower level of macrophage activation in these patients. [ABSTRACT FROM AUTHOR]

Published

2016

11. Letter: retreatment of patients with chronic hepatitis C who have failed interferon-free combination therapy with direct acting anti-virals.

Author

Kozbial, K., Aberle, S. W., Susser, S., Al‐Zoairy, R., Moser, S., Stättermayer, A. F., Maieron, A., Gschwantler, M., Stauber, R., Graziadei, I., Zoller, H., Beinhardt, S., Holzmann, H., Munda‐Steindl, P., Hofer, H., Sarrazin, C., and Ferenci, P.

Subjects

HEPATITIS C treatment, ANTIVIRAL agents, COMBINATION drug therapy, NUCLEOTIDE sequence, DRUG resistance in microorganisms

Abstract

Linked Content This article is linked to Majumdar et al paper. To view this article visit https://doi.org/10.1111/apt.13633. [ABSTRACT FROM AUTHOR]

Published

2017

12. The present and future disease burden of hepatitis C virus (HCV) infection with today's treatment paradigm.

Author

Razavi, H., Waked, I., Sarrazin, C., Myers, R. P., Idilman, R., Calinas, F., Vogel, W., Mendes Correa, M. C., Hézode, C., Lázaro, P., Akarca, U., Aleman, S., Balık, İ., Berg, T., Bihl, F., Bilodeau, M., Blasco, A. J., Brandão Mello, C. E., Bruggmann, P., and Buti, M.

Subjects

HEPATITIS C virus, VIREMIA, VIRUS diseases, LIVER diseases, TREATMENT effectiveness, NUMBER systems

Abstract

The disease burden of hepatitis C virus ( HCV) is expected to increase as the infected population ages. A modelling approach was used to estimate the total number of viremic infections, diagnosed, treated and new infections in 2013. In addition, the model was used to estimate the change in the total number of HCV infections, the disease progression and mortality in 2013-2030. Finally, expert panel consensus was used to capture current treatment practices in each country. Using today's treatment paradigm, the total number of HCV infections is projected to decline or remain flat in all countries studied. However, in the same time period, the number of individuals with late-stage liver disease is projected to increase. This study concluded that the current treatment rate and efficacy are not sufficient to manage the disease burden of HCV. Thus, alternative strategies are required to keep the number of HCV individuals with advanced liver disease and liver-related deaths from increasing. [ABSTRACT FROM AUTHOR]

Published

2014

13. 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

14. Serum micro RNA-122 kinetics in patients with chronic hepatitis C virus infection during antiviral therapy.

Author

Köberle, V., Waidmann, O., Kronenberger, B., Andrei, A., Susser, S., Füller, C., Perner, D., Zeuzem, S., Sarrazin, C., and Piiper, A.

Subjects

MICRORNA, HEPATITIS C treatment, ANTIVIRAL agents, INTERFERONS, LIVER injuries

Abstract

The levels of the liver-specific micro RNA-122 (mi R-122) circulating extracellularly in the blood have been shown to be increased upon liver damage. However, it is unknown if the levels of serum mi R-122 are altered during antiviral therapy and reflect the therapeutic success. Here, we investigated mi R-122 serum levels in patients with chronic hepatitis C virus ( HCV) genotype 1 infection during antiviral therapy with pegylated interferon and ribavirin. Therefore, sera from 60 patients with chronic HCV infection genotype 1 showing sustained virological response ( SVR), non-response or relapse to therapy obtained at baseline, 4, 12, 24 weeks, end of treatment and follow-up were analysed retrospectively for mi R-122 content by quantitative real-time reverse transcription PCR. The time courses of mi R-122 were correlated with HCV RNA as well as standard liver parameters. We found that while there was no relation between serum mi R-122 and HCV RNA levels at baseline, the decline in HCV RNA upon beginning of the therapy closely correlated with the reduction of serum mi R-122 in the three different patient groups. Moreover, the serum mi R-122 level correlated well with alanine aminotransaminase, a marker of ongoing liver damage. At follow-up serum mi R-122 levels remained low in SVR, but increased to baseline levels in patients not responding or showing relapse to therapy. In contrast, the serum concentration of the ubiquitously expressed mi R-16 did not change during therapy. We conclude that the serum level of mi R-122 well reflects the success of interferon/ribavirin therapy in patients with chronic HCV infection. [ABSTRACT FROM AUTHOR]

Published

2013

15. Dynamics of hepatitis B virus quasispecies heterogeneity and virologic response in patients receiving low-to-moderate genetic barrier nucleoside analogs.

Author

Peveling‐Oberhag, J., Herrmann, E., Kronenberger, B., Farnik, H., Susser, S., Sarrazin, C., Zeuzem, S., and Hofmann, W.‐P.

Subjects

HEPATITIS B virus, VIROLOGY, NUCLEOSIDES, LAMIVUDINE, ANTIVIRAL agents, DNA, REVERSE transcriptase

Abstract

We characterized the early dynamics of hepatitis B virus ( HBV) quasispecies evolution during the first weeks of antiviral therapy with low-to-moderate genetic barrier antiviral drugs and associated these data with antiviral response patterns. Fifteen chronic hepatitis B patients (men, 10; mean age, 34; HBe Ag positive, 6) who received lamivudine or telbivudine for at least 52 weeks were included. HBV DNA was extracted from serum, and a 910-bp fragment covering domains A-F of the reverse transcriptase region was amplified, cloned and sequenced. Parameters of quasispecies heterogeneity, genetic diversity and complexity were calculated and were correlated with complete virologic response, defined as undetectable HBV DNA at week 52. Nine patients achieved complete virologic response during the observational period. While baseline HBV DNA levels and HBeAg status were associated with virologic response, baseline quasispecies complexity and diversity of responders showed no significant difference to those of nonresponders ( P > 0.05). However, at week 4, quasispecies complexity of nonresponders was significantly higher compared with that of responders on the nucleotide level ( P = 0.01) and the aa level ( P = 0.04). The number of synonymous substitutions per synonymous site dropped significantly in responders at week 4 ( P = 0.04), while there was no difference in nonresponders. The HBV quasispecies complexity at the early stage of antiviral therapy (week 4) with the low-to-moderate genetic barrier nucleoside analogs lamivudine or telbivudine was associated with subsequent virologic response. Further studies are needed to confirm HBV quasispecies evolution as additional predictive marker for beneficial treatment outcome. [ABSTRACT FROM AUTHOR]

Published

2013

16. Acoustic radiation force impulse imaging for non-invasive assessment of liver fibrosis in chronic hepatitis B.

Author

Friedrich‐Rust, M., Buggisch, P., Knegt, R. J., Dries, V., Shi, Y., Matschenz, K., Schneider, M. D., Herrmann, E., Petersen, J., Schulze, F., Zeuzem, S., and Sarrazin, C.

Subjects

ACOUSTIC radiation force impulse imaging, NONINVASIVE diagnostic tests, FIBROSIS, LIVER disease diagnosis, CHRONIC hepatitis B, LIVER physiology

Abstract

Acoustic radiation force impulse ( ARFI) imaging is a novel ultrasound-based elastography method that is integrated in a conventional ultrasound machine. It might provide an alternative method to transient elastography for the noninvasive assessment of liver fibrosis. While previous studies have shown comparable diagnostic accuracy of ARFI to transient elastography in chronic hepatitis C, the aim of the present prospective multicenter study was to evaluate ARFI for the assessment of liver fibrosis in chronic hepatitis B. ARFI imaging involves the mechanical excitation of tissue using short-duration acoustic pulses to generate localized displacements in tissue. The displacements result in shear-wave propagation which is tracked using ultrasonic, correlation-based methods and recorded in m/s. In the present international prospective study, patients infected with chronic hepatitis B received ARFI imaging, blood tests and if available transient elastography. The results were compared to liver biopsy as reference method analysed by a central pathologist. In 92 of 114 patients, a comparison of ARFI with transient elastography was possible. ARFI imaging and transient elastography correlated significantly with histological fibrosis stage. The diagnostic accuracy expressed as areas under ROC curves for ARFI imaging and transient elastography was 0.75 and 0.83 for the diagnosis of significant fibrosis ( F ≥ 2), 0.93 and 0.94 for the diagnosis of severe fibrosis ( F ≥ 3), and 0.97 and 0.93 for the diagnosis of liver cirrhosis, respectively. No significant difference was found between ARFI and transient elastography. ARFI imaging is a reliable ultrasound-based method for the assessment of advanced stages of liver fibrosis in chronic hepatitis B. [ABSTRACT FROM AUTHOR]

Published

2013

17. Modulation of replication efficacy of the hepatitis C virus replicon Con1 by site-directed mutagenesis of an NS4B aminoterminal basic leucine zipper.

Author

Welker, M.-W., Susser, S., Welsch, C., Perner, D., Füller, C., Kronenberger, B., Herrmann, E., Zeuzem, S., and Sarrazin, C.

Subjects

VIRAL replication, HEPATITIS C virus, HEPATITIS C, MUTAGENESIS, VIRAL proteins, MICROBIAL mutation, PROTEIN-protein interactions

Abstract

. The hepatitis C virus (HCV) nonstructural protein 4B (NS4B) is assumed to function as a membrane anchor and protein hub for the viral replication complex. The aim of the current work was to modulate HCV replication efficacy in the subgenomic Con1 replicon by mutations of specific sites within the aminoterminal-located basic leucine zipper (bZIP), a candidate motif for protein-protein interactions involving NS4B. Mutational sites and amino acid substitutes were determined by in-silico sequence analyses of the NS4B-bZIP motif in 357 isolates of HCV genotype 1b from the euHCVdB and LosAlamos database and consecutive analysis of conserved physico-chemical properties at bZIP specific positions. Mutants with predicted minor, medium or major reduction of replication efficacy were tested in the pFKI389neo/NS3-3′/ET plasmid replicon model. Four sites (L25, T29, V39 and W43) of crucial importance for bZIP-mediated protein interaction with predicted apolarity of respective amino acid positions were selected for mutational studies. Substitutes with physico-chemical properties matching the predicted requirements either well (T29A), moderately (L25W, V39W), or insufficiently (T29E, W43E) were associated with slightly improved, moderate and marked decreased replication efficacy, respectively. Spontaneous (T29G) and adaptive (A28G, E40G) mutations occurred in the T29E mutation isolate only and were associated with marked reduction of replication efficacy. The bZIP motif region of NS4B is crucial for RNA replication in the subgenomic Con1 replicon system. RNA replication efficacy can be modulated by site-directed mutagenesis at specific bZIP functional sites. New adaptive amino acid mutations were identified within the HCV NS4B protein. [ABSTRACT FROM AUTHOR]

Published

2012

18. High-dose silibinin rescue treatment for HCV-infected patients showing suboptimal virologic response to standard combination therapy.

Author

Biermer, M., Schlosser, B., Fülöp, B., van Bömmel, F., Brodzinski, A., Heyne, R., Keller, K., Sarrazin, C., and Berg, T.

Subjects

SILIBININ, DRUG dosage, HEPATITIS C virus, VIROLOGY, COMBINATION drug therapy, VIREMIA, ANTIVIRAL agents, FOLLOW-up studies (Medicine)

Abstract

. Incomplete suppression of hepatitis C virus (HCV) replication with persistence of minimal viremia (partial virologic response) leading to treatment failure can be observed in a significant proportion of HCV type 1-infected patients during antiviral therapy. Recently, high-dose intravenous silibinin has demonstrated strong antiviral activity against HCV. We were therefore interested in whether patients with partial virologic response can be rescued by the on-treatment addition of a short-term course of high-dose intravenous silibinin infusions. Twenty patients who failed to achieve a complete virologic response to different interferon-based regimens qualified for the rescue strategy and received 1400 mg/day silibinin infusions on two consecutive days. Complete viral suppression (below the limit of detection <6 IU/mL, TMA assay) could be induced in 13 of 20 patients within the first week after the short-term silibinin infusion, and all but one of them also remained HCV RNA negative during the subsequent follow-up period on continued peginterferon plus ribavirin treatment. In the remaining seven patients, no complete suppression could be achieved although four showed a significant HCV RNA reduction in response to silibinin. Silibinin infusions were generally well tolerated, and activation of abdominal peristalsis with nausea, diarrhoea and vomiting were the most prominent side effects. Of the twelve patients who exhibited a durable response to peginterferon and ribavirin treatment, three achieved an SVR, two achieved a week 12 SVR and four suffered a viral relapse. Three patients could not complete the assigned antiviral treatment with peginterferon alpha and ribavirin for nonvirological reasons. Short-term administration of high-dose intravenous silibinin might be an interesting approach to rescue patients with ongoing minimal residual viremia while on interferon-based therapy. These preliminary findings may stimulate further studies to evaluate more refined therapeutic strategies. [ABSTRACT FROM AUTHOR]

Published

2012

19. Mutations selected in the hepatitis C virus NS3 protease domain during sequential treatment with boceprevir with and without pegylated interferon alfa-2b.

Author

Vermehren, J., Susser, S., Lange, C. M., Forestier, N., Karey, U., Hughes, E., Ralston, R., Tong, X., Zeuzem, S., and Sarrazin, C.

Subjects

HEPATITIS C virus, INTERFERONS, PROTEASE inhibitors, GENETIC mutation, DRUG dosage, GLYCOPROTEINS, ENZYME inhibitors, FLAVIVIRUSES

Abstract

Summary. Treatment with hepatitis C virus (HCV)-NS3-protease inhibitors lead to the selection of resistant variants. Viral kinetics and resistance profiles in patients who are re-treated with the same protease inhibitor are unknown. Viral kinetics and NS3-resistance mutations obtained by clonal sequencing of the NS3-protease were analyzed in nine HCV-genotype-1-infected nonresponder patients who were sequentially treated with boceprevir (400 mg t.i.d.) for 1 week, peginterferon-alfa-2b for 2 weeks and combination of the two for 2 weeks in varying order. In addition to predominant wild-type isolates, previously described boceprevir-resistant mutations (V36, T54, R155, A156, V170) were observed. Furthermore, two resistant mutations (Q41, F43) were detected for the first time in vivo. In three patients, mutations selected after initial treatment with boceprevir were re-selected during subsequent boceprevir exposure. However, mutational patterns after the first and second exposure to boceprevir were different in five patients. In one patient, a viral variant (V55A) known to reduce susceptibility to boceprevir was the predominant variant observed at baseline and throughout treatment and was associated with a shallow viral decline. Different resistance mutations were selected during treatment with boceprevir ± peginterferon. Sequential short-term dosing of boceprevir was not associated with accumulation of resistant variants but pre-existing variants may impair virologic response. [ABSTRACT FROM AUTHOR]

Published

2012

20. Comparison of Envelope 2 CD81 binding regions in PBMC-derived versus serum-derived hepatitis C virus isolates: higher conservation of CD81 region 2 in PBMC isolates.

Author

Welker, M.-W., Welsch, C., Ochs, D., Hofmann, W. P., Herrmann, E., Piiper, A., Hartmann, R. W., Zeuzem, S., Sarrazin, C., and Kronenberger, B.

Subjects

HEPATITIS C virus, VIRAL hepatitis, BLOOD testing, RNA viruses, CD antigens, GENETIC mutation, BINDING sites

Abstract

The aim of the present study was to investigate the variability of hepatitis C virus (HCV) CD81 binding regions (CD81-1/2) in peripheral blood mononuclear cells (PBMC)-derived and serum-derived HCV-RNA samples. HCV-RNA was isolated from PBMC (10 cells) and serum samples from 37 patients chronically infected with HCV genotype 1a/1b ( n = 21/16). The hypervariable regions 1/2 (amino acid 384-410, amino acid 474-482) and regions CD81-1/2 (amino acid 474-494, amino acid 522-551) were analysed. Mutational frequency of amino acid sequences was compared between PBMC-derived and serum-derived HCV variants as well as local accumulation of mutations. Furthermore, CD81 was quantified on PBMC. Mutational frequency was not different between PBMC-derived and serum-derived HCV variants. A trend to lower mutational frequency in genotype 1a PBMC variants compared with serum-derived variants was observed in region CD81-2 (5% vs 10%). Smoothed mutational frequency analysis showed a significantly lower variability within genotype 1a CD81-2 in PBMC-derived compared to serum-derived HCV-RNA ( P = 0.026). CD81 expression on PBMC was not correlated with the number of mutations within the CD81 binding regions. Conclusion: A higher conservation was observed in region CD81-2 in PBMC-derived versus serum-derived HCV-RNA indicating selection of HCV variants on PBMC. The variability in the CD81 binding regions appeared to be independent from CD81 expression. [ABSTRACT FROM AUTHOR]

Published

2011

21. Review article: specifically targeted anti-viral therapy for hepatitis C – a new era in therapy.

Author

Lange, C. M., Sarrazin, C., and Zeuzem, S.

Subjects

*HEPATITIS C, *GASTROENTEROLOGY, *RIBAVIRIN, *CLINICAL trials, *GENETIC research, *LIVER diseases

Abstract

Aliment Pharmacol Ther 2010; 32: 14–28 Background Novel, directly acting anti-viral agents, also named ‘specifically targeted anti-viral therapy for hepatitis C’ (STAT-C) compounds, are currently under development. Aim To review the potential of STAT-C agents which are currently under clinical development, with a focus on agents that target HCV proteins. Methods Studies evaluating STAT-C compounds were identified by systematic literature search using PubMed as well as databases of abstracts presented in English at recent liver and gastroenterology congresses. Results Numerous directly-acting anti-viral agents are currently under clinical phase I–III evaluation. Final results of phase II clinical trials evaluating the most advanced compounds telaprevir and boceprevir indicate that the addition of these NS3/4A protease inhibitors to pegylated interferon-alfa and ribavirin strongly improves the chance to achieve a SVR in treatment-naive HCV genotype 1 patient as well as in prior nonresponders and relapsers to standard therapy. Monotherapy with directly acting anti-virals is not suitable. NS5B polymerase inhibitors in general have a lower anti-viral efficacy than protease inhibitors. Conclusions STAT-C compounds in addition to pegylated interferon-alfa and ribavirin can improve SVR rates at least in HCV genotype 1 patients. Future research needs to evaluate whether a SVR can be achieved by combination therapies of STAT-C compounds in interferon-free regimens. [ABSTRACT FROM AUTHOR]

Published

2010

22. 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

23. Expert opinion on the treatment of patients with chronic hepatitis C.

Author

Zeuzem, S., Berg, T., Moeller, B., Hinrichsen, H., Mauss, S., Wedemeyer, H., Sarrazin, C., Hueppe, D., Zehnter, E., and Manns, M. P.

Subjects

HEPATITIS C virus, THERAPEUTICS, INTERFERONS, RIBAVIRIN, PATIENTS, CLINICAL trials

Abstract

The current preferred treatment for patients with hepatitis C virus (HCV) is combination therapy consisting of pegylated interferon alfa and ribavirin (RBV) for 24–48 weeks. Although this approach appears to be highly effective for patients with HCV genotypes 2 or 3, who have a sustained virological response (SVR) of approximately 80%, the treatment algorithm is less effective for patients with HCV genotype 1, as these patients have SVR rates of just 40–50%. In order to improve treatment outcomes, this article explores potential approaches for the optimization of treatment for patients with HCV genotype 1: considering shorter treatment periods for patients with a rapid virological response (RVR), increasing treatment periods for slow responders, and increasing RBV dose are all suggestions. Results from clinical trials suggest that approximately 20% of the HCV genotype 1-infected population are slow responders, and around 15% of all HCV genotype-1 infected patients could benefit from a shorter treatment duration without compromising the SVR rate. Interest has also focused on whether treatment duration could be individualized in some patients with genotype 2 and 3 infection. Here all the findings from recent studies are translated into practical advice, to help practitioners make evidence-based treatment decisions in everyday clinical practice. Although there are areas where currently available data do not provide conclusive evidence to suggest amending treatment approaches, there is clearly potential for individualized treatment in all aspects of hepatitis treatment in the future. [ABSTRACT FROM AUTHOR]

Published

2009

24. 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

25. 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

26. Correlation of amino acid variations within nonstructural 4B protein with initial viral kinetics during interferon-alpha-based therapy in HCV-1b-infected patients.

Author

Welker, M.-W., Hofmann, W.-P., Welsch, C., von Wagner, M., Herrmann, E., Lengauer, T., Zeuzem, S., and Sarrazin, C.

Subjects

ANTIVIRAL agents, HEPATITIS C, LIVER diseases, GLYCOPROTEINS, ANTINEOPLASTIC agents

Abstract

Chronic hepatitis C is a major cause of liver cirrhosis leading to chronic liver failure and hepatocellular carcinoma. Different hepatitis C virus (HCV) proteins have been associated with resistance to interferon-alpha-based therapy. However, the exact mechanisms of virus-mediated interferon resistance are not completely understood. The importance of amino acid (aa) variations within the HCV nonstructural (NS)4B protein for replication efficiency and viral decline during the therapy is unknown. We investigated pretreatment sera from 42 patients with known outcome to interferon-based therapy. The complete NS4B gene was amplified and sequenced. Mutational analyses of predicted conformational, functional, structural and phylogenetic properties of the deduced aa sequences were performed. The complete NS4B protein was highly conserved with a median frequency of 0.015 ± 0.009 aa exchanges (median ± SD, 4.00 ± 2.31). Especially within the predicted transmembranous domains of the NS4B protein, the mean number of aa variations was low (median frequency, 0.013 ± 0.013). Neither the number of aa variations nor specific aa exchanges were correlated with HCV RNA serum concentration at baseline. A rapid initial HCV RNA decline of ≥1.5 log10 IU/mL at week 2 of interferon-based therapy was associated with a higher frequency of nonconservative aa exchanges within the complete NS4B protein in comparison with patients with a nonrapid HCV RNA decline (median frequency, 0.011 ± 0.005 vs 0.004 ± 0.003, P = 0.006). Overall, the aa sequence of the NS4B protein was highly conserved, indicating an important role for replication in vivo. Amino acid variations with relevant changes of physicochemical properties may influence replication efficiency, associated with a rapid early virological response. [ABSTRACT FROM AUTHOR]

Published

2007

27. Induction of hepatitis C virus (HCV)-specific T cells by needle stick injury in the absence of HCV-viraemia.

Author

Kubitschke, A., Bahr, M. J., Aslan, N., Bader, C., Tillmann, H. L., Sarrazin, C., Greten, T., Wiegand, J., Manns, M. P., and Wedemeyer, H.

Subjects

T cells, HEPATITIS C virus, INFECTIOUS disease transmission, NATURAL immunity, CELLULAR immunity, MEDICAL virology

Abstract

Background The risk of hepatitis C virus (HCV) infection after occupational exposure is low with seroconversion rates between 0 and 5%. However, factors associated with natural resistance against HCV after needle stick injury are poorly defined. HCV-specific T-cell responses have been described in cross-sectional studies of exposed HCV-seronegative individuals. Materials and methods In this study, we prospectively followed 10 healthcare professionals who experienced an injury with an HCV-contaminated needle. Blood samples were taken on the day or the day after the event and at different time points during follow-up for up to 32 months. HCV-specific T-cell responses were investigated directly ex vivo and in T-cell lines. Results None of the individuals became positive for HCV-RNA in serum tested with the highly sensitive transcription-mediated amplification (TMA)-assay or in peripheral blood mononuclear cells (PBMC). All of them remained anti-HCV negative throughout follow-up. At the time of injury, HCV-specific CD4+ T-cell responses were already detectable in two individuals and became detectable thereafter in three additional persons. Transient HCV-specific CD8+ T-cell responses developed in two HLA-A2 positive patients, which became negative until the most recent follow-up after 5 and 17 months, respectively. Conclusion We demonstrate the development of HCV-specific T cells in HCV-exposed individuals after needle stick injury indicating subinfectious exposure to HCV. T-cell immunity against HCV may contribute to the low prevalence of HCV in medical healthcare professionals in Western countries. [ABSTRACT FROM AUTHOR]

Published

2007

28. Impaired health-related quality of life in patients with chronic hepatitis C and persistently normal aminotransferase levels.

Author

von Wagner, M., Lee, J.-H., Kronenberger, B., Friedl, R., Sarrazin, C., Teuber, G., Herrmann, E., and Zeuzem, S.

Subjects

HEPATITIS C, VIRAL hepatitis, QUALITY of life, AMINOTRANSFERASES, LIVER diseases

Abstract

A significant impact of hepatitis C virus (HCV) infection on health-related quality of life (HRQOL) has been previously described. However, comprehensive data on the quality of life in patients with chronic hepatitis C and persistently normal aminotransferase levels (PNAL) are currently not available. One hundred fifteen patients with chronic hepatitis C (45 with persistently normal aminotransferases and 70 with elevated aminotransferases) and 50 healthy subjects were enrolled. Emotional and psychological states were assessed by Profile of Mood States (POMS) scale and HRQOL was assessed by the ‘Everyday Life’ questionnaire (EDLQ), a validated questionnaire related to the SF-36 Health Survey. An impairment in HRQOL was observed in patients with chronic hepatitis C showing PNAL compared with healthy subjects with significant differences for the factor scores depression and anger in the POMS scale as well as for the items body, relationship to partner, self-confidence and zest of life in the EDLQ. No differences in any questionnaire were observed between patients with chronic hepatitis C showing PNAL or elevated aminotransferase levels except of a worse mean level for factor score anger in POMS scale in patients with persistently normal aminotransferases. No association of quality of life with severity of liver disease was found. Impairment of HRQOL by chronic infection with HCV is similar in patients with PNAL and those with elevated aminotransferase levels. [ABSTRACT FROM AUTHOR]

Published

2006

29. 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

30. 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

31. 13C-methacetin breath test as liver function test in patients with chronic hepatitis C virus infection.

Author

Braden, B., Faust, D., Sarrazin, U., Zeuzem, S., Dietrich, C. F., Caspary, W. F., and Sarrazin, C.

Subjects

BREATH tests, HEPATITIS C, CYTOCHROME P-450, VIRAL hepatitis, LIVER diseases, BLOOD alcohol analysis

Abstract

: The13C-methacetin breath test enables the quantitative evaluation of the cytochrome P450-dependentliver function.: To find out whether this breath test is sensitive in noncirrhotic patients also with chronic hepatitis C in early stages of fibrosis.: Sixty-one healthy controls and 81 patients with chronic hepatitis C underwent a13C-methacetin breath test. In all patients, a liver biopsy was performed. The liver histology was classified according to the histology activity index–Knodell score.: Delta over baseline values of the patients at 15 min significantly differed from controls (19.2 ± 9.2‰ vs. 24.1 ± 5.7‰;P < 0.003). The cumulative recovery after 30 min in patients was 11.4 ± 4.8% and in healthy controls 13.8 ± 2.8% (P < 0.002). However, patients with early fibrosis (histology activity index IVB) did not differ in delta over baseline values of the patients at 15 min (23.2 ± 7.9‰ vs. 22.6 ± 7.2‰;P = 0.61) or cumulative recovery (13.6 ± 3.7% vs. 13.2 ± 3.8%;P = 0.45) from patients with more advanced fibrosis (histology activity index IVC). Patients with clinically nonsymptomatic cirrhosis (histology activity index IVD; Child A) metabolized13C-methacetin to a significantly lesser extent (delta over baseline values of the patients at 15 min: 8.3 ± 4.9‰;P < 0.005 and cumulative recovery after 30 min: 5.6 ± 3.2%;P < 0.003). The13C-methacetin breath test identified cirrhotic patients with 95.0% sensitivity and 96.7% specificity.: The non-invasive13C-methacetin breath test reliably distinguishes between early cirrhotic (Child A) and noncirrhotic patients, but fails to detect early stages of fibrosis in patients with chronic hepatitis C. [ABSTRACT FROM AUTHOR]

Published

2005

32. Mutations in the putative HCV-E2 CD81 binding regions and correlation with cell surface CD81 expression.

Author

Kronenberger, B., Sarrazin, C., Hofmann, W.P., von Wagner, M., Herrmann, E., Welsch, C., Elez, R., Rüster, B., Piiper, A., and Zeuzem, S.

Subjects

*HEPATITIS C, *CD antigens, *CELL receptors, *LIVER diseases, *LYMPHOCYTES

Abstract

The hepatitis C virus (HCV) envelope (E)2 protein interacts with the cellular receptor CD81 leading to modulation of B and T cell function. Recently, a higher binding affinity of subtype 1a in comparison with 1b derived E2 proteins for CD81 in vitro was described. The importance of mutations within the putative CD81 binding regions of different HCV geno-/subtypes in correlation with CD81 expression is unknown. In the present study, CD81 expression on blood lymphocytes of patients with chronic hepatitis C infected with different HCV geno-/subtypes were analysed by fluorescence activated cell sorter analyses. In addition, the putative CD81 binding regions on the E2 gene comprising the hypervariable region (HVR)2 were analysed by direct sequencing. CD81 expression on CD8(+) T-lymphocytes from patients infected with subtype 1a ( n = 6) was significantly higher in comparison with subtype 1b ( n = 12) and 3 ( n = 5) infected patients before and during antiviral therapy ( P = 0.006; P = 0.021, respectively). Sequencing of the putative CD81 binding regions in the E2 protein comprising the HVR2 (codon 474–495 and 522–552 according to the HCV-1a prototype HCV-H) showed a highly conserved motif within HVR2 for subtype 1a isolates and an overall low number of mutations within the putative CD81 binding regions, whereas numerous mutations were detected for subtype 1b isolates (12.0 vs 23.6%). HCV-3 isolates showed an intermediate number of mutations within the putative binding sites (19.2%; P = 0.022). In conclusion, the highly conserved sequence within HVR2 and putative CD81 binding sites of subtype 1a isolates previously associated with a high CD81 binding affinity in vitro is correlated with high CD81 expression on CD8(+) T-lymphocytes in vivo. [ABSTRACT FROM AUTHOR]

Published

2004

33. Dynamics of hepatitis C virus quasispecies turnover during interferon- α treatment.

Author

von Wagner, M., Lee, J.-H., Ruster, B., Kronenberger, B., Sarrazin, C., Roth, W.K., and Zeuzem, S.

Subjects

HEPATITIS C virus, INTERFERONS, THERAPEUTICS, SERUM

Abstract

Interferon- α (IFN) has been shown to accelerate the evolution of hepatitis C virus (HCV) variants (quasispecies) in nonresponder patients. Different sensitivities of HCV variants to IFN are discussed as a possible mechanism. In the present study, quasispecies were investigated in detail by a newly established and validated direct solid-phase sequencing of the hypervariable region 1 (HVR1), during the initial 3 months of IFN therapy. According to single strand conformation polymorphism (SSCP) analysis, 14 of 26 (54%) virologic nonresponders with quasispecies evolution were identified. Six representative patients with SSCP changes were selected for frequent HVR1 sequencing. Pre-existing variants were identified by cloning and sequencing of the pretreatment serum HCV sample. In one patient the major type was substituted by a minor variant within 3 days of treatment while in the majority of patients the pretreatment major type did not decline before days 26–57 of treatment. Total serum HCV RNA levels remained constant in all patients. In conclusion, although quasispecies evolution during IFN therapy is common, it occurs after a wide range of time intervals after initiation of therapy. Thus, nonresponse to IFN cannot exclusively be explained by changes in the quasispecies. [ABSTRACT FROM AUTHOR]

Published

2003

34. ELECTRON BACKSCATTERING PATTERN IDENTIFICATION OF SURFACE MORPHOLOGY OF FATIGUE CRACKS IN TA6V.

Author

Sarrazin, C., Chiron, R., Lesterlin, S., and Petit, J.

Published

1994

35. Letter: telaprevir triple therapy in chronic hepatitis C genotype 1 patients receiving haemodialysis.

Author

Wiegand, J., Maasoumy, B., Buggisch, P., Buslau, A., Schiefke, I., Berg, T., Wedemeyer, H., Sarrazin, C., and Hinrichsen, H.

Subjects

CHRONIC hepatitis C, THERAPEUTICS

Abstract

A letter to the editor is presented in response to the article "The clinical significance of drug-drug interactions in the era of direct-acting anti-viral agents against chronic hepatitis C" by B. Maasoumy, K. Port, and S. B. Calle in the 2013; 38 issue.

Published

2014

36. Letter: impact of HBV genotypes and PC/BCP mutations on serum HBsAg levels in Chinese HBeAg negative patients—Authors′ reply.

Author

Kuhnhenn, L., Jiang, B., Kubesch, A., Zeuzem, S., Sarrazin, C., Hildt, E., and Peffer, K.‐H.

Subjects

HEPATITIS B virus, GENOTYPES

Published

2018

37. Editorial: HBsAg serum levels in HBeAg‐negative chronic HBV infection—is it a matter of genotype? Authors’ reply.

Author

Kuhnhenn, L., Jiang, B., Kubesch, A., Zeuzem, S., Sarrazin, C., Hildt, E., and Peiffer, K.‐H.

Subjects

CELL surface antigens, HEPATITIS B virus, SERUM, GENOTYPES, GENETIC mutation

Abstract

The article discusses the serum level of HBsAg in HBeAg-negative chronic hepatitis B virus (HBV) infection. Topics mention including the impacts of the HBV genotype and frequent mutation in HBV DNA and qHBsAg level, evaluating and understanding the molecular virology and composition of the secreted HBsAg.

Published

2018

38. Editorial: genotype 3 HCV—who still needs ribavirin in a pan‐genotypic era? Authors’ reply.

Author

von Felden, J., Vermehren, J., Schulze zur Wiesch, J., Sarrazin, C., and Christensen, S.

Subjects

SOFOSBUVIR, HEPATITIS C, RIBAVIRIN, MEDICAL microbiology, GENOTYPES

Abstract

The article presents the authors' response to comments on their study "High efficacy of sofosbuvir/velpatasvir and impact of baseline resistance-associated substitutions in hepatitis C genotype 3 infection," which appeared in a 2018 issue. The authors note that the study was assessed for the prevalence of high level NS5A RASs as too low to draw meaningful conclusions regarding their impact on treatment outcome.

Published

2018

39. NO ASSOCIATION BETWEEN COMPLEMENT FACTOR 5 VARIANTS AND PROGRESSIVE LIVER FIBROSIS IN HEPATITIS C VIRUS INFECTION.

Author

Halangk, J, Sarrazin, C, Puhl, G, Neumann, K, Berg, T, and Witt, H

Published

2006

40. ChemInform Abstract: Stress Corrosion Behavior of Molybdenum Implanted Stainless Steel.

Author

SARRAZIN, C., DESJARDINS, D., and OLIVE, J. M.

Published

1991

41. Impaired HBsAg release and antiproliferative/antioxidant cell regulation by HBeAg-negative patient isolates reflects an evolutionary process.

Author

Basic M, Thiyagarajah K, Glitscher M, Schollmeier A, Wu Q, Görgülü E, Lembeck P, Sonnenberg J, Dietz J, Finkelmeier F, Praktiknjo M, Trebicka J, Zeuzem S, Sarrazin C, Hildt E, and Peiffer KH

Subjects

Humans, Cell Proliferation, Virus Replication, Hepatitis B, Chronic virology, NF-E2-Related Factor 2 metabolism, NF-E2-Related Factor 2 genetics, Mutation, Genotype, Antioxidants metabolism, Antioxidant Response Elements genetics, Hepatitis B Surface Antigens genetics, Hepatitis B Surface Antigens metabolism, Hepatitis B e Antigens metabolism, Hepatitis B virus genetics

Abstract

Background: The hepatitis B e antigen (HBeAg)-negative infection Phase 3 is characterized by no or minimal signs of hepatic inflammation and the absence of hepatic fibrosis. However, underlying molecular mechanisms leading to this benign phenotype are poorly understood., Methods: Genotype A, B and D HBeAg-negative patient isolates with precore mutation G1896A from Phase 3 were analysed in comparison with respective HBeAg-positive rescue mutant and HBeAg-positive wild-type reference genomes regarding differences in viral replication, morphogenesis, infectivity and impact on NF-E2-related factor 2 (Nrf2)/antioxidant response element (ARE)-dependent gene expression and cellular kinome., Results: In comparison with reference genomes, the patient isolates are characterized by a lower intra- and extracellular hepatitis B surface antigen (HBsAg)-amount, and HBsAg-retention in the endoplasmic reticulum. Rescue of HBeAg expression increased HBsAg-amount but not its release. Expression of the isolated genomes is associated with a higher Nrf2/ARE-dependent gene expression as compared to reference genomes independent of HBeAg expression. Kinome analyses revealed a decreased activity of receptors involved in regulation of proliferative pathways for all patient isolates compared to the reference genomes. No specific conserved mutations could be found between all genomes from Phase 3., Conclusions: HBeAg-negative genomes from Phase 3 exhibit distinct molecular characteristics leading to lower HBsAg synthesis and release, enhanced oxidative stress protection and decreased activity of key kinases, triggering an antiproliferative stage, which might contribute to the lower probability of hepatocellular carcinoma. The observed differences cannot be associated with loss of HBeAg or specific mutations common to all analysed isolates, indicating the phenotype of Phase 3 derived genomes to be the result of a multifactorial process likely reflecting a conserved natural selection process., (© 2024 The Author(s). Liver International published by John Wiley & Sons Ltd.)

Published

2024

42. Not uncommon: HBV genotype G co-infections among healthy European HBV carriers with genotype A and E infection.

Author

Basic M, Kubesch A, Kuhnhenn L, Görgülü E, Finkelmeier F, Dietz J, Knabe M, Mücke VT, Mücke MM, Berger A, Zeuzem S, Sarrazin C, Hildt E, and Peiffer KH

Subjects

DNA, Viral genetics, Genotype, Hepatitis B Surface Antigens genetics, Hepatitis B virus genetics, Humans, Liver Cirrhosis, Coinfection epidemiology

Abstract

Background & Aims: HBV genotype G (HBV/G) is mainly found in co-infections with other HBV genotypes and was identified as an independent risk factor for liver fibrosis. This study aimed to analyse the prevalence of HBV/G co-infections in healthy European HBV carriers and to characterize the crosstalk of HBV/G with other genotypes., Methods: A total of 560 European HBV carriers were tested via HBV/G-specific PCR for HBV/G co-infections. Quasispecies distribution was analysed via deep sequencing, and the clinical phenotype was characterized regarding qHBsAg-/HBV-DNA levels and frequent mutations. Replicative capacity and expression of HBsAg/core was studied in hepatoma cells co-expressing HBV/G with either HBV/A, HBV/D or HBV/E using bicistronic vectors., Results: Although no HBV/G co-infection was found by routine genotyping PCR, HBV/G was detected by specific PCR in 4%-8% of patients infected with either HBV/A or HBV/E but only infrequently in other genotypes. In contrast to HBV/E, HBV/G was found as the quasispecies major variant in co-infections with HBV/A. No differences in the clinical phenotype were observed for HBV/G co-infections. In vitro RNA and DNA levels were comparable among all genotypes, but expression and release of HBsAg was reduced in co-expression of HBV/G with HBV/E. In co-expression with HBV/A and HBV/E expression of HBV/G-specific core was enhanced while core expression from the corresponding genotype was markedly diminished., Conclusions: HBV/G co-infections are common in European inactive carriers with HBV/A and HBV/E infection, but sufficient detection depends strongly on the assay. HBV/G regulated core expression might play a critical role for survival of HBV/G in co-infections., (© 2021 The Authors. Liver International published by John Wiley & Sons Ltd.)

Published

2021

43. Treatment outcomes in hepatitis C virus genotype 1a infected patients with and without baseline NS5A resistance-associated substitutions.

Author

Dietz J, Vermehren J, Matschenz K, Buggisch P, Klinker H, Schulze Zur Wiesch J, Hinrichsen H, Peiffer KH, Graf C, Discher T, Trauth J, Schattenberg JM, Piecha F, Mauss S, Niederau C, Müller T, Neumann-Haefelin C, Berg CP, Zeuzem S, and Sarrazin C

Abstract

Background&aims: The presence of baseline resistance-associated substitutions (RASs) reduced sustained virologic response (SVR) rates in chronic hepatitis C virus (HCV) genotype 1a infected patients treated with Elbasvir/Grazoprevir (EBR/GZR). This study aimed to evaluate the frequency of NS5A RASs and treatment outcomes in patients for whom EBR/GZR was intended., Methods: We sequenced NS5A in 832 samples from German genotype1a-infected DAA-naïve patients population-based, which were collected in the European Resistance Database. Treatment outcomes and clinical parameters were evaluated in 519 of these patients retrospectively., Results: Overall, 6.5% of patients harbored EBR-specific NS5A RASs at baseline, including Q30H/R (3.3%), L31M (1.8%), Y93H (1.6%) and other individual variants. Antiviral treatment, including EBR/GZR, was initiated in 88% of patients. In the absence of RASs, the majority of patients received EBR/GZR for 12 weeks (57%) and the SVR rate was 97% compared to 99% SVR achieved using other DAA regimens (LDV/SOF±RBV, G/P, PrOD+RBV, VEL/SOF). Various regimens were used in the presence of RASs and SVR rates were high following treatment with LDV/SOF (100%), G/P (83%), PrOD/RBV (100%), VEL/SOF (100%), SMV/SOF (100%) and EBR/GZR+RBV for 16 weeks (100%). However, two patients received EBR/GZR for 16 weeks without RBV and one relapsed., Conclusions: EBR/GZR treatment with or without RBV for 12 or 16 weeks according to a baseline RAS analysis was highly effective with ≥97% SVR in patients with genotype 1a. EBR/GZR without RBV should be avoided in patients with RASs. High SVR rates were also achieved using other 8 or 12 weeks DAA regimens., (This article is protected by copyright. All rights reserved.)

Published

2020

44. Serum sphingolipids predict de novo hepatocellular carcinoma in hepatitis C cirrhotic patients with sustained virologic response.

Author

Mücke VT, Thomas D, Mücke MM, Waidmann O, Zeuzem S, Sarrazin C, Pfeilschifter J, Vermehren J, Finkelmeier F, and Grammatikos G

Subjects

Adult, Aged, Aged, 80 and over, Biomarkers, Tumor blood, Carcinoma, Hepatocellular virology, Female, Germany, Hepatitis C, Chronic complications, Humans, Liver Cirrhosis virology, Liver Neoplasms virology, Logistic Models, Male, Middle Aged, Predictive Value of Tests, Retrospective Studies, Risk Factors, Sustained Virologic Response, alpha-Fetoproteins analysis, Antiviral Agents therapeutic use, Carcinoma, Hepatocellular blood, Hepatitis C, Chronic drug therapy, Liver Cirrhosis complications, Liver Neoplasms blood, Sphingolipids blood

Abstract

Background & Aims: Curing hepatitis C virus (HCV) infection reduces the risk of hepatocellular carcinoma (HCC) development, yet HCC occurs despite sustained virologic response (SVR) in 2%-8% of cirrhotic patients. Sphingolipids (SLs) have been identified as new biomarkers of chronic liver disease and HCC. The aim of this study was to evaluate serum SLs as diagnostic HCC biomarkers in patients with HCV-associated cirrhosis at SVR12., Methods: From 2014 to 2016, 166 patients with HCV-cirrhosis and SVR were recruited and SL profiles were measured at baseline and 12 weeks after completion of direct-acting antiviral (DAA) therapy. All patients received HCC surveillance in line with current guideline recommendations. Minimum follow-up period comprised 6 months., Results: Our study included 130 (78%) patients without history of HCC, 25 (15%) with history of HCC prior DAA therapy and 11 (7%) patients with de novo HCC after FU12. In those with upcoming de novo HCC serum C24DHC (P = 0.006), C24:1DHC (P = 0.048) and C16Cer (P = 0.011) were significantly upregulated at FU12, but not AFP (P = 0.138). Contemporaneous ultrasound did not visualize HCC, at this time. C16Cer stayed sole independent predictor with high diagnostic accuracy of AFP-positive (AUC = 0.741) and -negative (AUC = 0.766) HCC development. Serum SL parameters decreased from baseline to SVR12., Conclusions: C24DHC, C24:1DHC and especially C16Cer were superior to AFP in early detection of AFP-positive and -negative de novo HCC development. We observed significant SL profile changes upon SVR. SLs may play a role in non-invasive HCC surveillance and hepatocarcinogenesis., (© 2019 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2019

45. Clinical significance of detectable and quantifiable HCV RNA at the end of treatment with ledipasvir/sofosbuvir in GT1 patients.

Author

Maasoumy B, Buggisch P, Mauss S, Boeker KHW, Müller T, Günther R, Zimmermann T, Manns MP, Sarrazin C, Hüppe D, Wedemeyer H, and Vermehren J

Subjects

Female, Germany, Hepacivirus genetics, Humans, Male, Registries, Retrospective Studies, Sofosbuvir, Sustained Virologic Response, Uridine Monophosphate therapeutic use, Viral Load, Antiviral Agents therapeutic use, Benzimidazoles therapeutic use, Fluorenes therapeutic use, Hepatitis C drug therapy, RNA, Viral isolation & purification, Ribavirin therapeutic use, Uridine Monophosphate analogs & derivatives

Abstract

Background & Aims: AASLD/IDSA treatment guidelines for hepatitis C virus (HCV) infection state that testing for quantitative HCV RNA can be considered at the end of antiviral treatment (EOT) with interferon-free regimens. However, it remains unclear how to respond to a detectable or even quantifiable HCV RNA result. The aim of this study was to analyse the frequency and predictive value of detectable and quantifiable HCV RNA results at the EOT in patients with HCV genotype 1 infection treated with ledipasvir (LDV) and sofosbuvir (SOF) ± ribavirin (RBV) in a large real-world cohort., Methods: A retrospective analysis of the DHC-R (Deutsches Hepatitis C-Register, German Hepatitis C-Registry) cohort was performed including all patients who were treated with LDV/SOF ± RBV and in whom HCV RNA testing was done with either the Roche COBAS AmpliPrep/COBAS TaqMan (CAP/CTM) or the Abbott RealTime HCV assay (ART)., Results: The frequency of detectable HCV RNA at the EOT was 7% in this real-world study involving 471 patients. Furthermore, 3% of the patients (n = 14/471) even had quantifiable viral load at the EOT. Detectable and quantifiable results were more frequent if the ART was used for testing. However, SVR was achieved by 32/33 patients (97%) with detectable and even by all 14 patients (100%) with quantifiable HCV RNA results at the EOT., Conclusion: Detectable and even quantifiable HCV RNA results are quite frequent if highly sensitive HCV RNA assays are used. However, treatment prolongation is not indicated, as SVR rates remain high in these patients., (© 2018 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2018

46. Treatment of HCV genotype 2 with sofosbuvir and ribavirin results in lower sustained virological response rates in real life than expected from clinical trials.

Author

Tacke F, Günther R, Buggisch P, Klinker H, Schober A, John C, Lutz T, Pfeiffer-Vornkahl H, Niederau C, Cornberg M, Sarrazin C, and Mauss S

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Drug Therapy, Combination, Female, Germany, Hepacivirus genetics, Humans, Liver Cirrhosis virology, Logistic Models, Male, Middle Aged, Prospective Studies, RNA, Viral, Registries, Sustained Virologic Response, Young Adult, Antiviral Agents administration & dosage, Hepatitis C, Chronic drug therapy, Ribavirin administration & dosage, Sofosbuvir administration & dosage

Abstract

Background and Aims: Hepatitis C virus (HCV) infections with genotype 2 (GT2) are generally considered as easy to treat. The current standard therapy is 12 weeks of sofosbuvir and ribavirin. However, sustained virological response (SVR) rates varied substantially in distinct subgroups. Therefore, re-assessing the efficacy of interferon-free therapy in cohorts with larger patient numbers is warranted., Methods: The German Hepatitis C registry is a national multicenter cohort. Patients are treated at the discretion of the physician. Data are collected by a web-based data system and confirmed by plausibility checks and on-site monitoring., Results: A total of 265 (4.3%) of 6034 patients enrolled in the registry were infected with GT2, and 236 had initiated treatment (60% males, 98% Caucasian, median age 54 years). Treatment with sofosbuvir and ribavirin for 12 weeks achieved SVR at week 12 post-treatment (SVR12) in 136/164 (83%) patients. SVR12 rates for this regimen were 80% (35/44) in treatment-experienced patients, 74% (20/27) in cirrhotics and 75% (21/28) in patients with HCV-RNA ≥6 million IU/mL. The overall SVR rate in patients treated with sofosbuvir/ribavirin 12 weeks per protocol (PP), excluding therapy discontinuation or lost to follow-up, was 135/151 (89%). PP SVR12 rates were 91% for treatment naïve, 83% for cirrhotic and 80% for treatment-experienced patients respectively., Conclusions: In this large GT2 cohort, sofosbuvir and ribavirin for 12 weeks achieved lower SVR rates compared to treatment outcomes expected from phase 3 trials. These findings highlight the need for establishing alternative treatment strategies for GT2 patients, especially in patients with unfavourable outcome factors., (© 2016 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2017

47. Apolipoprotein E allele frequencies in chronic and self-limited hepatitis C suggest a protective effect of APOE4 in the course of hepatitis C virus infection.

Author

Mueller T, Fischer J, Gessner R, Rosendahl J, Böhm S, van Bömmel F, Knop V, Sarrazin C, Witt H, Marques AM, Kovacs P, Schleinitz D, Stumvoll M, Blüher M, Bugert P, Schott E, and Berg T

Subjects

Adult, Aged, Aged, 80 and over, Case-Control Studies, Female, Fibrosis, Genetic Predisposition to Disease, Germany, Hepacivirus, Humans, Lipoproteins, LDL blood, Liver pathology, Male, Middle Aged, Polymorphism, Single Nucleotide, Young Adult, Apolipoproteins E genetics, Gene Frequency, Hepatitis C, Chronic genetics

Abstract

Background & Aims: Infectious hepatitis C virus (HCV) particles bind to host lipoproteins such as low-density lipoproteins (LDLs). Low-density lipoprotein receptors (LDLR) have been termed candidate receptors for HCV-LDL complexes. Functional host genetic single nucleotide polymorphisms (SNPs) in the apolipoprotein E (APOE) gene encoding apolipoprotein E (apoE) - a major structural LDL component and natural ligand of LDLR - likely influence the course of HCV infection. We investigated the prevalence of APOE SNPs in two large and independent cohorts of patients with chronic HCV infection compared to respective controls., Methods: We genotyped 996 chronically HCV-infected patients; 179 patients with spontaneous HCV clearance; 283 individuals with non-HCV-associated liver disease; and 2 234 healthy controls., Results: APOE genotype proportions in patients with persistent HCV infection significantly differed from healthy controls (P = 0.007) primarily because of a substantial under-representation of APOE4 alleles in chronically HCV-infected patients (10.2%) compared to 13.0% in healthy controls (P = 0.001). The distribution of APOE4 allele positive genotypes (ε2ε4, ε3ε4, ε4ε4) also significantly differed between chronically HCV-infected patients and healthy controls (1.4%, 17%, 1% vs. 2.4%, 20.5%, 1.7%; P = 0.001), suggesting a protective effect of the APOE4 allele in HCV infection. This was confirmed by a significant over-representation of the APOE4 allele in patients with spontaneous HCV clearance (17.6%; P = 0.00008). The APOE4 allele distribution in patients with non-HCV-associated liver disease (14.0%) was very similar to healthy controls and also differed from chronically HCV-infected patients (P = 0.012), suggesting HCV specificity., Conclusions: Our findings suggest that the APOE4 allele may confer a protective effect in the course of HCV infection., (© 2016 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2016

48. Telaprevir drug monitoring during antiviral therapy of hepatitis C graft infection after liver transplantation.

Author

Farnik H, Zimmermann T, Herrmann E, Bechstein WO, Kronenberger B, Galle PR, Labocha S, Ferreiros N, Geisslinger G, Zeuzem S, Sarrazin C, and Welker MW

Subjects

Antiviral Agents therapeutic use, Chromatography, Liquid, Drug Therapy, Combination, Humans, Interferon-alpha therapeutic use, Liver Transplantation methods, Oligopeptides therapeutic use, Polyethylene Glycols therapeutic use, Prospective Studies, Recombinant Proteins therapeutic use, Recurrence, Ribavirin therapeutic use, Statistics, Nonparametric, Tandem Mass Spectrometry, Antiviral Agents blood, Drug Monitoring methods, Hepatitis C drug therapy, Immunosuppression Therapy methods, Liver Transplantation adverse effects, Oligopeptides blood, Tacrolimus therapeutic use

Abstract

Background & Aims: Recurrence of hepatitis C virus (HCV) infection after orthotopical liver transplantation (OLT) is common and associated with reduced graft and patient survival. The protease inhibitor telaprevir may enhance virological response rates in patients after OLT in combination with pegylated interferon-alfa and ribavirin. Pharmacokinetic studies have shown significant drug-drug interactions between telaprevir and immunosuppression (IS), but telaprevir pharmacokinetics in OLT patients with IS are unknown. Aim of the present study was to analyse telaprevir plasma concentrations in patients with HCV genotype 1 infection after OLT in comparison to patients without OLT and IS., Methods: Five patients with HCV genotype 1 infection after OLT and 37 HCV genotype 1-infected patients patients without prior OLT were treated with telaprevir 2250 mg daily, ribavirin 1000/1200 mg daily and pegylated interferon-alfa-2a 180 μg once weekly (triple therapy). Telaprevir plasma concentrations were analysed by liquid chromatography-electrospray-ionization-tandem mass spectrometry. HCV RNA was assessed by automatized reverse-transcription polymerase chain-reaction., Results: Median (range) telaprevir plasma concentrations of TW 4, 8 and 12 were 3970 (1980-4430) ng/ml and 2520 (1870-8730) ng/ml in patients after OLT and ciclosporin- or tacrolimus-based IS, respectively, as compared to 2790 (1870-3140) in non-OLT patients (P = 0.3). In one patient with tacrolimus-based IS, telaprevir dose had to be adjusted to achieve virological response. Telaprevir plasma concentrations were steady at treatment weeks 4, 8 and 12 in patients with and without IS., Conclusions: Telaprevir drug monitoring may be necessary in patients with tacrolimus-based IS in patients with HCV graft infection after OLT., (© 2014 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2015

49. Comparison of acoustic radiation force impulse imaging with transient elastography for the detection of complications in patients with cirrhosis.

Author

Vermehren J, Polta A, Zimmermann O, Herrmann E, Poynard T, Hofmann WP, Bojunga J, Sarrazin C, Zeuzem S, and Friedrich-Rust M

Subjects

Adult, Aged, Biomarkers metabolism, Carcinoma, Hepatocellular complications, Carcinoma, Hepatocellular metabolism, End Stage Liver Disease complications, End Stage Liver Disease metabolism, Esophageal and Gastric Varices etiology, Esophageal and Gastric Varices metabolism, Female, Fibrosis complications, Fibrosis diagnosis, Fibrosis metabolism, Humans, Liver Cirrhosis complications, Liver Cirrhosis metabolism, Liver Neoplasms complications, Liver Neoplasms metabolism, Male, Middle Aged, Predictive Value of Tests, Reagent Kits, Diagnostic, Carcinoma, Hepatocellular diagnosis, Elasticity Imaging Techniques methods, End Stage Liver Disease diagnosis, Esophageal and Gastric Varices diagnosis, Liver Cirrhosis diagnosis, Liver Neoplasms diagnosis

Abstract

Background: Acoustic radiation force impulse (ARFI) imaging is a new non-invasive, ultrasound-based method for the evaluation of liver fibrosis and cirrhosis., Aim: To determine the diagnostic accuracy of ARFI imaging, transient elastography (TE) and Fibrotest for the evaluation of complications in patients with cirrhosis., Methods: A total of 166 patients (109 male, mean age: 54 ± 11 years) with chronic liver disease and established cirrhosis were included in this study. ARFI-imaging of the liver and spleen, TE and Fibrotest were performed in all patients. In addition, clinical, laboratory and morphological parameters, including MELD/Child-Pugh scores, presence of oesophageal varices and hepatocellular carcinoma, history of variceal bleeding and history of hepatic encephalopathy were recorded., Results: Acoustic radiation force impulse liver was significantly correlated with ARFI spleen (r = 0.48, P < 0.001), TE (r = 0.75, P < 0.001) and Fibrotest (r = 0.21, P = 0.006). The diagnostic accuracy (AUROC) for the diagnosis of large oesophageal varices was 0.58 (95% CI: 0.48-0.67), 0.58 (0.49-0.67), 0.53 (0.44-0.63) and 0.50 (0.41-0.59) for ARFI liver, spleen, TE and Fibrotest respectively (P > 0.20). The AUROC for the detection of hepatocellular carcinoma (HCC) was 0.54 (0.39-0.70), 0.58 (0.44-0.73), 0.56 (0.40-0.73) and 0.72 (0.60-0.84) respectively (P > 0.20). Multiple logistic regression analysis showed that ARFI spleen better predicted the presence of large oesophageal varices and HCC compared with ARFI liver., Conclusions: The diagnostic accuracy of ARFI liver and spleen was comparable to TE and Fibrotest for the detection of complications in patients with cirrhosis., (© 2011 John Wiley & Sons A/S.)

Published

2012

50. Future treatment of chronic hepatitis C with direct acting antivirals: is resistance important?

Author

Halfon P and Sarrazin C

Subjects

Antiviral Agents therapeutic use, Drug Resistance, Viral genetics, Hepacivirus genetics, Hepatitis C, Chronic virology, Host-Pathogen Interactions, Humans, Mutation, Serine Proteinase Inhibitors therapeutic use, Viral Nonstructural Proteins antagonists & inhibitors, Viral Nonstructural Proteins drug effects, Viral Nonstructural Proteins genetics, Virus Replication drug effects, Virus Replication genetics, Antiviral Agents pharmacology, Drug Resistance, Viral drug effects, Hepacivirus drug effects, Hepatitis C, Chronic drug therapy, Serine Proteinase Inhibitors pharmacology

Abstract

Recent advances in molecular biology have led to the development of novel small molecules that target specific viral proteins of the hepatitis C virus (HCV) life cycle. These drugs, collectively termed directly acting antivirals (DAA), include a range of non-structural (NS) 3/NS4A protease, NS5B polymerase and NS5A inhibitors at various stages of clinical development. Some others drugs called 'non DAA'or indirect inhibitors are not focused on one site of the life cycle target and are still in early pre-clinical and clinical phase I, II and III trials. The rapid replication rate of HCV, along with the low fidelity of its polymerase, results in a generation of mutations throughout the viral genome and sequence variation in the HCV population known as a quasispecies. The efficacy of DAA is limited by the presence of these mutations, resulting in amino acid substitutions within the targeted proteins which affect viral sensitivity to these compounds. Thus, attributable to the high genetic variability of HCV, variants with reduced susceptibility to DAA can occur naturally even before treatment begins, but usually at low levels. Thus it is not surprising that these changes are selected in patients that either breakthrough or do not respond to potent DAA treatment. Six major position mutations in the NS3 HCV Protease (36, 54, 155, 156, 168 and 170), fifteen in the NS5B polymerase (96, 282, 316, 365, 414, 419, 423, 448, 482, 494, 495, 496, 499, 554, 559) and five in the NS5 A region (28, 30, 31, 58 and 93) have now been reported in vitro or in vivo associated with different levels of resistance. The amino acid composition at several of the drug resistance sites can vary between the HCV genotypes/subtypes, resulting in different consensus amino acids leading to a reduction in replicative fitness as well as reduced DAA and non- DAA sensitivity. Information on patterns of resistance to and cross resistance between antiviral agents is increasingly available and may be important for decisions on how to combine drugs to achieve an optimum antiviral effect. This review debates the clinical relevance of resistance to direct and indirect inhibitors taking into account the future potential therapeutic strategies to help patients who do develop resistance to HCV inhibitors. Finally, this chapter treats two points of view: 'for' and 'against' the question of the importance of resistance., (© 2012 John Wiley & Sons A/S.)

Published

2012