Impact of new DAA therapy on real clinical practice: A multicenter region-wide cohort study

Simone Lanini, Paola Scognamiglio, Alessandra Mecozzi, Lorella Lombardozzi, Vincenzo Vullo, Mario Angelico, Antonio Gasbarrini, Gloria Taliani, Adolfo Francesco Attili, Carlo Federico Perno, Adriano De Santis, Vincenzo Puro, Fabio Cerqua, Gianpiero D'Offizi, Adriano Pellicelli, Orlando Armignacco, Francesco Saverio Mennini, Massimo Siciliano, Enrico Girardi, Vincenzo PanellaGiuseppe Ippolito, C. Sarrecchia, M. D. Di Paolo, S. Francioso, A. Brega, I. Lenci, L. Sarmati, Maurizio Pompili, Antonio Grieco, Enrica Tamburrini, R. Apaccini, Luca Miele, G. D'Ettorre, I. Mezzaroma, C. Furlan, D. Accapezzato, F. Paoletti, M. Merili, S. Corradini, S. Sereno, C. Fimiani, C. Mastropietro, G. Labbadia, G. Gentile, Giuseppe Gentile, C. Pasquazzi, M. Marignani, R. Guarisco, C. Puoti, L. Spilabotti, M. Montalbano, E. Boumis, U. Visco-Comandini, M. Zaccarelli, A. Ammassari, R. Lionetti, S. Murachelli, L. Loiacono, A. Antinori, Armando Antinori, P. Noto, F. Palmieri, S. Cicalini, S. Cerilli, A. Sampaolesi, L. Vincenzi, R. Bellagamba, V. Galati, A. Abdeddaim, F. Iacomi, G. Iannicelli, C. Mastroianni, Chiara Mastroianni, M. Lichtner, L. Ridola, T. Coluzzi, V. Mercurio, C. Del Borgo, L. Fondacaro, G. Cerasari, P. Guarascio, C. D'Ambrosio, G. Starnini, A. Caterini, R. Villani, Emanuele Rocco Villani, L. Sarracino, K. Casinelli, A. Moretti, U. Vespasiani, G. Galati, R. Cecere, M. Bonaventura, M. Scudieri

Research output: Contribution to journalArticle

13 Citations (Scopus)

Abstract

Background: Management of chronic hepatitis C (CHC) has significantly accelerated in the last few years. Currently, second generation direct acting antivirals (DAAs) promise clearance of infection in most of patients. Here we present the results of the first analysis carried out on data of Lazio clinical network for DAAs. Methods: The study was designed as a multicenter cohort: a) to assess the evolution of treatment during the first 24 months of the activity of the Clinical Network; b) to report overall efficacy of treatments; c) to analyze potential factors associated with lack of virological response at 12 weeks after therapy (SVR12); d) to evaluate the variation of ALT at baseline and 12 weeks after therapy in those who achieved SVR12 in comparison to those who did not. Analyses of efficacy were carried out with multilevel mixed effect logistic regression model. ALT temporal variation was assessed by mixed effect model mixed models with random intercept at patient's level and random slope at the level of the time; i.e. either before or after therapy. Results: Between 30 December 2014 and 31 December 2016 5279 patients started a DAA treatment; of those, 5127 (in 14 clinical centers) had completed the 12-week follow-up. Overall proportion of SVR12 was 93.41% (N = 4780) with no heterogeneity between the 14 clinical centers. Interruption as the consequence of severe side effect was very low (only 23 patients). Unadjusted analysis indicates that proportion of SVR12 significantly changes according to patient's baseline characteristics, however after adjusting for potential confounders only adherence to current guidelines, stage of liver diseases, gender, transplant and HIV status were independently associated with the response to therapy. Analysis of ALT temporal variation showed that ALT level normalized in most, but not, all patients who achieved SVR12. Conclusion: Our study confirmed the extraordinary efficacy of DAAs outside clinical trials. The advantage of DAAs was particularly significant for those patients who were previously considered as difficult-to-treat and did not have treatment options before DAAs era. Intervention based on network of select centers and prioritization of patients according to diseases severity was successful. Further studies are needed to establish whether clearance of HCV after DAAs therapy can arrest or even revert liver fibrosis in non-cirrhotic patients and/or improve life quality and expectancy in those who achieve SVR12 with cirrhosis.
Original languageEnglish
Pages (from-to)223-223
Number of pages1
JournalBMC Infectious Diseases
Volume18
DOIs
Publication statusPublished - 2018

Keywords

  • Adult
  • Aged
  • Aged, 80 and over
  • Antiviral Agents
  • Chronic hepatitis C
  • Clinical study
  • Cohort Studies
  • Direct acting antiviral
  • Drug Therapy, Combination
  • Drugs, Investigational
  • Female
  • Follow-Up Studies
  • Hepatitis C virus
  • Hepatitis C, Chronic
  • Humans
  • Infectious Diseases
  • Liver Cirrhosis
  • Liver cirrhosis
  • Liver damage
  • Male
  • Middle Aged
  • Mixed effect model
  • Multicenter cohort study
  • New therapy
  • Therapies, Investigational
  • Treatment efficacy

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