Combined therapy with interferon and low-dose ribavirin in posttransplantation recurrent hepatitis C: A pragmatic study

Key Points 1. Treatment of established recurrent hepatitis C with interferon-␣ monotherapy does not achieve sustained virologic response (SVR). 2. Treatment of established recurrent hepatitis C with combination interferon plus ribavirin achieves SVR rates of 17% to 27%, but dropout rates approach 30%. 3. Pretransplant prophylaxis against recurrent hepatitis C with combination interferon plus ribavirin is poorly tolerated in patients with decompensated hepatitis C cirrhosis. 4. Posttransplant prophylaxis with combination interferon plus ribavirin prevents both recurrent viremia and hepatitis in 15% to 20% of patients, but dropout rates approach 50%. 5. Hepatitis C virus genotype is the best predictor of response to antiviral prophylaxis and treatment of recurrent hepatitis C. 6. Interferon-␣ therapy is not associated with an increased risk of allograft rejection in liver transplant recipients. 7. Ribavirin therapy is associated with increased hemolysis in liver transplant recipients. 8. Preliminary data suggest pegylated interferon monotherapy will have similar efficacy but better tolerability than combination interferon plus ribavirin. 9. In a recent study, posttransplant immunoprophylaxis with polyclonal hepatitis C immunoglobulin had no effect on recurrent viremia or hepatitis. (Liver Transpl 2002;8: S28-S37.)

Section: Safety Issuesmentioning

confidence: 99%

“…4). [31][32][33][34][35][36][37][38][39] Unfortunately, between 20% and 50% 37 of patients were unable to complete treatment because of drug-related serious adverse events. …”

Section: Ribavirinmentioning

confidence: 99%

Section: Safety Issuesmentioning

confidence: 99%

See 1 more Smart Citation

Treatment of recurrent hepatitis C

Gane

2002

“…To prevent morbidity and mortality associated with recurrent hepatitis C, many centers have used interferon alfa (IFN-␣) and/or ribavirin (RVN) as either antiviral prophylaxis or treatment of established hepatitis C or hepatitis B. Regimens have ranged from monotherapies with RVN, [8][9][10][11][12][13][14] standard IFN-␣ , 9,[15][16][17][18][19][20][21][22][23][24][25][26][27][28][29] or pegylated IFN [30][31][32] to combination therapies with a standard IFN-␣ and RVN 27,29,[33][34][35][36][37][38][39][40][41][42][43][44][45][46][47][48][49][50][51][52] or pegylated IFN-␣ and RVN. 53 H...…”

mentioning

confidence: 99%

The clinical and immunologic impact of using interferon and ribavirin in the immunosuppressed host

Braun

Vierling

2003

C irrhosis caused by chronic hepatitis C virus (HCV) infection is the leading indication for cadaver and living donor liver transplantation. 1 Recurrent HCV infection, which occurs within days in virtually all allografts, is associated with a 10-to 20-fold increase in serum HCV RNA levels because of enhanced replication stimulated by immunosuppression. 2,3 A majority develop acute hepatitis C 1 to 4 months post-orthotopic liver transplantation (OLT) that is characterized by lymphocytic infiltration and hepatocyte apoptosis. Progression to chronic hepatitis C is associated with: (1) decline in HCV RNA levels observed in the acute phase because of effects of HCVspecific CD4 T helper subtype 1 (T H 1) and CD8 cell responses, (2) profibrotic effects of interferon-␥ (IFN-␥), and (3) proapoptotic effects of increased hepatocyte expression of Fas. 3 Progression of chronic hepatitis C is accelerated in immunosuppressed patients post OLT, resulting in a cumulative probability of cirrhosis in 30% by 5 years. 4 In addition, a minority develop severe, usually fatal, cholestatic hepatitis C within the first 6 months after OLT that is characterized by a direct cytopathic effect of excessive intrahepatic replication of HVC, intrahepatic anti-inflammatory T H 2 cytokine expression, and absence of an HCV-specific immune response. 3 Studies of the impact of different immunosuppressive regimens on recurrent hepatitis C also have been performed in an attempt to reduce hepatitis C progression while preventing acute cellular rejection (ACR). 5 Overall, HCV infection significantly reduces graft and patient survival compared with patients who undergo OLT for non-HCV-related indications. 6 Results of re-OLT are poor, 7 and this is an increasingly unrealistic option in view of the shortage of organ donors.To prevent morbidity and mortality associated with recurrent hepatitis C, many centers have used interferon alfa (IFN-␣) and/or ribavirin (RVN) as either antiviral prophylaxis or treatment of established hepatitis C or hepatitis B. Regimens have ranged from

“…With few exceptions, most studies have been nonrandomized. [13][14][15][16][17][18][19][20][21][22][23][24][25][26][27][28][29][30] Side effects are common, and dose reduction and withdrawals are seen in up to half of the patients. Furthermore, many patients require support to maintain hemoglobin and white cell count.…”

Section: Treatment Of Established Hepatitismentioning

confidence: 99%

Treatment of hepatitis C virus infection in the allograft

Neuberger

2003

Key Points 1. Recurrence of hepatitis C virus (HCV) in the graft is associated with a reduced quality of life and worse graft survival. 2. Pretransplantation, the severity of HCV recurrence may be reduced by reducing the pretransplantation load, by avoiding the use of organs from older donors, and by reducing the ischemic times. The effect of split livers on recurrence rates is uncertain. 3. The optimal immunosuppression regime has not been established but a heavy induction regime and treatment for acute rejection are associated with more viral replication and more graft damage. 4. Presently, there is no convincing evidence for preemptive treatment of HCV. 5. There are many studies on the effect of interferon with and without ribavirin for the treatment of HCV hepatitis. However, few are prospective, randomized, and controlled. 6. The current best treatment is with pegylated interferon and ribavirin; the dose and duration of treatment need to be established. Side-effects of treatment are common and reduction/withdrawal is frequent, but the regime is costeffective. 7. The role of newer treatments remains to be established. (Liver Transpl 2003;9:S101-S108.)I nfection of the liver allograft with hepatitis C virus (HCV) is associated with graft fibrosis, cirrhosis, and graft loss and a reduced quality of life. 1,2 The success of combination therapy with pegylated interferon and ribavirin in the treatment of HCV in the native liver and the development of newer and potentially more effective treatments has encouraged clinicians to treat recurrent HCV. Treatment of the Patient With HCVThe treatment of patients with HCV cannot be totally evidence-based, but given the current data, the following approaches seem reasonable. Reduction of Severity of HCV RecurrenceDonor. Where possible, avoid using grafts from older donors, avoid prolonged warm and cold ischemic times, and avoid using split livers (from cadaveric or living donors). It is appreciated that this approach is not always possible.Pretransplantation reduction of HCV load. given the side effects of treatment and the uncertainty of timing of transplantation, the balance seems against routine use of interferon to reduce viral load Avoidance of factors that may exacerbate viral damage. it seems sensible to avoid those factors that exacerbate HCV-related damage in the native liver, such as obesity, hyperglycemia, and alcohol. Immunosuppression RegimenOverimmunosuppression leads not only to an increased risk of sepsis, malignancy, and drug-specific complications, but will also enhance viral replication. Conversely, too little immunosuppression will lead to an increased risk of rejection (early acute rejection has little if any adverse impact on the graft), but the increased immunosuppression required to control such an episode will enhance viral replication. The optimal immunosuppressive regimen for such patients is discussed elsewhere in this issue.