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TREATMENT OF RECURRENT HCV INFECTION AFTER LIVER TRANSPLANTATION

TAJANA FILIPEC KANIŽAJ ; Klinička bolnica Merkur, Medicinski fakultet Sveučilišta u Zagrebu, Klinika za unutarnje bolesti, Zavod za gastroenterologiju, Zagreb, Hrvatska
VESNA ČOLIĆ-CVRLJE ; Klinička bolnica Merkur, Medicinski fakultet Sveučilišta u Zagrebu, Klinika za unutarnje bolesti, Zavod za gastroenterologiju, Zagreb, Hrvatska
ANNA MRZLJAK ; Klinička bolnica Merkur, Medicinski fakultet Sveučilišta u Zagrebu, Klinika za unutarnje bolesti, Zavod za gastroenterologiju, Zagreb, Hrvatska
RAJKO OSTOJIĆ ; Klinički bolnički centar Zagreb, Medicinski fakultet Sveučilišta u Zagrebu, Klinika za unutarnje bolesti, Zavod za gastroenterologiju, Zagreb, Hrvatska


Puni tekst: hrvatski pdf 141 Kb

str. 373-380

preuzimanja: 947

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Sažetak

Recurrent infection with HCV after liver transplantation (LT) is almost universal and is associated with substantial morbidity, mortality and graft loss. In contrast to immunocompetent individuals, HCV infection in immunosuppressed transplant recipients usually has an accelerated course. Acute hepatitis develops in approximately 75% of HCV recipients in the first six months following LT. Within the five years after LT, over 80% of HCV-infected liver transplant recipients develop histologic evidence of chronic allograft injury secondary to HCV, with up to 30% of cirrhosis. While the choice of calcineurin inhibitors has not clearly shown to affect the histologic HCV recurrence or the frequency of rejection in HCV-infected recipients, the cumulative exposure to corticosteroids is associated with increased mortality, higher levels of HCV viremia, and more severe histologic recurrence. Successful therapy has been shown to have a positive impact on both graft and patient survival. Combination therapy with interferon (pegylated and non-pegylated forms) plus ribavirin appears to provide maximum benefits. Drug therapy is usually administered for recurrent disease. No prophylactic therapy is available. Preemptive regimens offer no distinctive advantages over treatments for recurrent disease. Overall, treatment is poorly tolerated, with frequent need for dose reductions, especially due to cytopenias, and drug discontinuation in up to 50% of patients. Optimizing drug doses is important in maximizing sustained virologic response rates (SVR). The SVR achieved is between 33% and 42% in randomized studies treating patients with histologic recurrence. The potential factors that influence this low SVR rate are: 1) genotype 1 virus; 2) high viral load; 3) prior nonresponding to therapy; 4) side effects of antiviral treatment; 5) use of growth factors; and 6) effect of immunosuppression. In post-transplant patients with recurrent HCV disease, combination peg alpha-2b or alpha-2a in standard dose and ribavirin (800-1200 mg either ab initio or as an increasing dose) regimen for 48 weeks was significantly better than no therapy but not than any other therapy.

Ključne riječi

HCV infection; liver transplantation; antiviral therapy

Hrčak ID:

113726

URI

https://hrcak.srce.hr/113726

Datum izdavanja:

14.1.2014.

Podaci na drugim jezicima: hrvatski

Posjeta: 1.987 *