Contributors: Cento, V.; Nguyen, T.; Di Carlo, D.; Biliotti, E.; Gianserra, L.; Lenci, I.; Di Paolo, D.; Calvaruso, V.; Teti, E.; Cerrone, M.; Romagnoli, D.; Melis, M.; Danieli, E.; Menzaghi, B.; Polilli, E.; Siciliano, M.; Nicolini, L.; Di Biagio, A.; Magni, C.; Bolis, M.; Antonucci, F.; Di Maio, V.; Alfieri, R.; Sarmati, L.; Casalino, P.; Bernardini, S.; Micheli, V.; Rizzardini, G.; Parruti, G.; Quirino, T.; Puoti, M.; Babudieri, S.; Monforte, A.; Andreoni, M.; Craxi, A.; Angelico, M.; Pasquazzi, C.; Taliani, G.; Guedj, J.; Perno, C.; Ceccherini-Silberstein, F.
نبذة مختصرة : Background: Intracellular HCV-RNA reduction is a proposed mechanism of action of direct-acting antivirals (DAAs), alternative to hepatocytes elimination by pegylated-interferon plus ribavirin (PR). We modeled ALT and HCV-RNA kinetics in cirrhotic patients treated with currently-used all-DAA combinations to evaluate their mode of action and cytotoxicity compared with telaprevir (TVR)+PR. Study design: Mathematical modeling of ALT and HCV-RNA kinetics was performed in 111 HCV-1 cirrhotic patients, 81 treated with all-DAA regimens and 30 with TVR+PR. Kinetic-models and Cox-analysis were used to assess determinants of ALT-decay and normalization. Results: HCV-RNA kinetics was biphasic, reflecting a mean effectiveness in blocking viral production >99.8%. The first-phase of viral-decline was faster in patients receiving NS5A-inhibitors compared to TVR+PR or sofosbuvir+simeprevir (p<0.001), reflecting higher efficacy in blocking assembly/secretion. The second-phase, noted δ and attributed to infected-cell loss, was faster in patients receiving TVR+PR or sofosbuvir+simeprevir compared to NS5A-inhibitors (0.27 vs 0.21 d-1, respectively, p = 0.0012). In contrast the rate of ALT-normalization, noted λ, was slower in patients receiving TVR+PR or sofosbuvir+simeprevir compared to NS5A-inhibitors (0.17 vs 0.27 d-1, respectively, p<0.001). There was no significant association between the second-phase of viral-decline and ALT normalization rate and, for a given level of viral reduction, ALT-normalization was more profound in patients receiving DAA, and NS5A in particular, than TVR+PR. Conclusions: Our data support a process of HCV-clearance by all-DAA regimens potentiated by NS5A-inhibitor, and less relying upon hepatocyte death than IFN-containing regimens. This may underline a process of "cell-cure" by DAAs, leading to a fast improvement of liver homeostasis.
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