Einfluss von Ribavirin auf die Dynamik der Hepatitis-C-Virämie bei Interferon-α-behandelten Patienten mit Response oder Nonresponse

 

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Zusammenfassung

Die IFNα-Ribavirin-Kombinationstherapie hat sich bei Patienten mit chronischer Hepatitis C gegenüber einer alleinigen IFNα-Therapie als überlegen erwiesen. In dieser Studie wurde deshalb untersucht, ob Ribavirin, dessen Wirkungsmechanismus unklar ist, einen zusätzlichen Effekt auf die Hepatitis-C-Virämie hat. Verglichen wurde die Dynamik der Hepatitis-C-Virämie zwischen Patienten, die entweder auf eine IFNα-Mono- oder Kombinationstherapie angesprochen, oder Patienten, die auf beide Therapieformen keine Response gezeigt hatten.

64 unvorbehandelte Patienten mit chronischer Hepatitis C hatten entweder 3 × 6 Mio. Einheiten IFNα-2a (Hoffmann-La Roche)/Woche (n = 34) oder IFNα plus Ribavirin (Meduna) (14 mg/kg/Tag) (n = 30) für 12 Wochen erhalten. 37 der 64 behandelten Patienten (58 %) wurden nach 3-monatiger Therapie HCV-RNA-negativ (= Responder; 17 [46 %] mit IFNα-Monotherapie und 20 [54 %] mit Kombinations­therapie). Die restlichen 27 Patienten blieben HCV-RNA-positiv (= Nonresponder; 13 [48 %] mit IFNα-Monotherapie und 14 [52 %] mit Kombinationstherapie). Die HCV-RNA-Konzentrationen (bDNA assay, Chiron) wurden vor und 1, 2, 4 und 12 Wochen nach Therapiebeginn bestimmt. Mittels nicht­radioaktiver Einzelstrang-Konformations-(SSCP)Analyse der hypervariablen Region des HCV wurde untersucht, inwieweit der initiale Abfall der Hepatitis-C-Virämie bei Nonresponder-Patienten mit Änderungen der Virus­population (Quasispeziesverteilung) einhergeht.

Bei den Respondern hatte die Ribavirintherapie keinen Einfluss auf den Abfall der Hepatitis-C-Virämie. Auch bei den Nonrespondern kam es unabhängig von der Therapieform in der ersten Therapiewoche (Phase 1) zu einem Rückgang der Virämie (im Mittel 10,0 ± 2,3 auf 5,5 ± 1,1 MEq/ml). Im ­weiteren Verlauf (Phase 2) kam es jedoch unter IFNα-Monotherapie zu einem Anstieg der Virämie, während unter ­Kombinationstherapie ein weiterer Rückgang der HCV-RNA Konzentrationen zu verzeichnen war (Woche 12: 7,5 ± 2,9 MEq/ml [IFNα-mono, n = 12] vs. 3,0 ± 0,5 MEq/ml ­[Kombination, n = 15]). Der initiale Abfall der Virämie zeigte jedoch bei allen Nonrespondern individuell deutliche Unterschiede (Spannweite der Abnahme von 0-98 %, verglichen mit der Ausgangsvirämie) und bei 5 der 27 Nonresponder kam es zu einer Abnahme ≥ 1 log (≥ 90 %). Mittels SSCP­Analyse konnte keine signifikante Korrelation zwischen ­Virämieverlauf und Änderungen der Viruspopulation (SSCP-Bandenmuster) hergestellt werden.

Unsere Beobachtungen zeigen, dass Ribavirin in Kombination mit IFNα einen zusätzlichen, jedoch erst verzögert (2-4 Wochen nach Therapiebeginn) einsetzenden antiviralen/immunmodulatorischen Effekt hat. Der auch bei den Nonrespondern zu beobachtende 2-phasige Virämieverlauf kann nicht allein durch die Selektion primär IFNα-resistenter HCV-Varianten erklärt werden. Die individuellen Unterschiede bezüglich der Dynamik der Hepatitis-C-Virämie bei IFNα-Nonrespondern legen eine Neubewertung der Definition von Nonresponse nahe.

Influence of ribavirin on the dynamics of hepatitis C ­viremia in interferon-α-treated patients with response or nonresponse

Combination therapy with interferon-α (IFNα) plus Ribavirin has been shown to improve the response rate in patients with chronic hepatitis C as compared to IFNα alone. However, the mode of anti-viral action of Ribavirin is still unknown. To prove, whether Ribavirin has any additional effect on the decline of hepatitis C viremia during the first weeks of treatment patients with and without combination therapy were compared. Kinetic studies were performed in patients who either responded to IFNα alone or IFNα plus ­Ribavirin combination as well as in nonresponders to both forms of therapeutic approaches.

64 IFNα naive patients with histologically proven chronic hepatitis C were included in the study. Patients were random­ized to receive either IFNα-2a (Hoffmann-La Roche) 6 MU thrice weekly or IFNα 6 MU tiw plus Ribavirin (Meduna) 14 mg/kg/day for 12 weeks. 37 patients (58 %) became HCV RNA-negative (= responders; 17 [46 %] with IFNα alone, and 20 [54 %] with combination therapy). 27 patients remained HCV RNA-positive (= non-responders; 13 [48 %] with ­IFNα alone, and 14 [52 %] with combination therapy). HCV RNA concentrations were measured in all patients at baseline as well as 1, 2, 4, and 12 weeks after the start of treatment (bDNA assay, Chiron). Using nonradioactive single-stranded conformation (SSCP)-analysis of the HCV hypervariable ­region 1 we investigated further whether initial viral decline is correlated with changes in viral quasispecies distribution.

In primary responders, ribavirin did not influence hepatitis C viremia decline which was of biphasic nature. Also in nonresponders HCV RNA levels decreased after one week of treatment irrespectively of the mode of therapy (mean 10.0 ± 2.3 to 5.5 ± 1.1) (phase 1). In the following weeks, how­ever, 2 types of HCV dynamics could be observed ­(phase 2). In patients with combination therapy, a further reduction of viremia level could be observed, whereas viremia levels in patients with IFNα alone slightly increased (week 12: 3.0 ± 0.5 MEq/mL [combination, n = 15] vs. 7.5 ± 2.9 MEq/mL [IFNα-mono, n = 12]). The individual response of these nonresponder patients showed, however, marked differ­ences (range percentage decline after 4 weeks, 0-98 %). Changes in the viral population (quasispecies distribution) as cause of these differences could be excluded by SSCP-analysis of PCR products of the HCV hypervariable region 1.

Ribavirin in combination with IFNα exerts an additional anti-viral/immunmodulatory effect which manifests itself in phase 2 of hepatitis C viremia decline. The biphasic decline of hepatitis C viremia also observed in IFNα-nonresponders can not be explained by the selection of primary IFNα-resistant viral variants. The individual differences in the dynamic of hepatitis C viremia observed in the so called „nonresponders” imply that the term „nonresponder” should be redefined, considering our observation that a marked viral decline can occur in these patients.

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Anschrift für die Verfasser:

Dr. med. Thomas Berg

Medizinische Klinik m. S. Hepatologie und Gastroenterologie Universitätsklinikum Charité Campus Virchow-Klinikum Humboldt-Universität

Augustenburger Platz 1

13353 Berlin

Email: thomas.berg@charite.de