Incidence and risk factors of early HCC occurrence in HCV patients treated with direct acting antivirals: a prospective multicentre study.
Aged
Antiviral Agents
/ therapeutic use
Carcinoma, Hepatocellular
/ epidemiology
Female
Hepatitis C, Chronic
/ complications
Humans
Incidence
Liver Cirrhosis
/ complications
Liver Neoplasms
/ epidemiology
Logistic Models
Male
Middle Aged
Multivariate Analysis
Prospective Studies
Risk Factors
Sustained Virologic Response
Direct acting antivirals
HCC
HCV cirrhosis
Immune-surveillance
Journal
Journal of translational medicine
ISSN: 1479-5876
Titre abrégé: J Transl Med
Pays: England
ID NLM: 101190741
Informations de publication
Date de publication:
28 08 2019
28 08 2019
Historique:
received:
20
04
2019
accepted:
18
08
2019
entrez:
30
8
2019
pubmed:
30
8
2019
medline:
17
7
2020
Statut:
epublish
Résumé
An unexpected increased HCC recurrence and occurrence rate among HCV patients treated with direct acting antivirals combination has been reported. Aim of the study was the evaluation of early HCC occurrence rate and its risk factors in a HCV infected population, treated with direct-acting-antivirals. According to the Italian ministerial guidelines for direct-acting-antivirals treatment, 1022 consecutive HCV patients treated with direct-acting-antivirals were enrolled. Patients either with active HCC at imaging or history of previous treated HCC, HBV or HIV co-infection, or liver transplant recipients were excluded. The SVR, defined as the persistent absence of detectable serum HCV-RNA 12 weeks after the end of treatment (SVR12), was assessed for all enrolled patients. Abdominal ultrasound was performed before starting antiviral therapy, and repeated every 6 months. HCC was diagnosed according to the international guidelines. Patients showing either nodular patterns suggestive of HCC or with uncertain dynamic vascular behaviour were excluded from a further follow-up. Nine hundred and eighty-five patients completed the 48 weeks follow-up after the end of treatment. A Sofosbuvir-based regimen was administered in the 74.9% of patients, among whom, the 71.6% underwent a simultaneous Ribavirin administration. A sustained virological response at 12 weeks off treatment was documented in 966 patients (98.2%). During the post treatment follow-up HCC was detected in 35 patients, with a cumulative incidence rate of the 3.55%. At multivariate analysis, four variables resulted independently associated with HCC development, both in a cirrhosis based and a class B Child based model, respectively: cirrhosis/class B Child, therapeutic schedule including Sofosbuvir without Ribavirin, liver stiffness values, male gender and presence of diabetes. A multivariate analysis performed on Child A cirrhotic patients, showed that Sofosbuvir based therapeutic treatment without Ribavirin had a HCC occurrence 5.7 higher than Ribavirin-based schedules with or without Sofosbuvir (p < 0.0001, OR: 5.686, 95% CI 2.455-13.169). Our data suggest that early HCC occurrence appears more frequently related to Sofosbuvir-based therapy without Ribavirin which, indeed, seems to play a protective role on HCC onset. Therefore, a careful follow-up should be mandatory, especially in those regimens including Sofosbuvir without Ribavirin.
Sections du résumé
BACKGROUND
An unexpected increased HCC recurrence and occurrence rate among HCV patients treated with direct acting antivirals combination has been reported. Aim of the study was the evaluation of early HCC occurrence rate and its risk factors in a HCV infected population, treated with direct-acting-antivirals.
METHODS
According to the Italian ministerial guidelines for direct-acting-antivirals treatment, 1022 consecutive HCV patients treated with direct-acting-antivirals were enrolled. Patients either with active HCC at imaging or history of previous treated HCC, HBV or HIV co-infection, or liver transplant recipients were excluded. The SVR, defined as the persistent absence of detectable serum HCV-RNA 12 weeks after the end of treatment (SVR12), was assessed for all enrolled patients. Abdominal ultrasound was performed before starting antiviral therapy, and repeated every 6 months. HCC was diagnosed according to the international guidelines. Patients showing either nodular patterns suggestive of HCC or with uncertain dynamic vascular behaviour were excluded from a further follow-up.
RESULTS
Nine hundred and eighty-five patients completed the 48 weeks follow-up after the end of treatment. A Sofosbuvir-based regimen was administered in the 74.9% of patients, among whom, the 71.6% underwent a simultaneous Ribavirin administration. A sustained virological response at 12 weeks off treatment was documented in 966 patients (98.2%). During the post treatment follow-up HCC was detected in 35 patients, with a cumulative incidence rate of the 3.55%. At multivariate analysis, four variables resulted independently associated with HCC development, both in a cirrhosis based and a class B Child based model, respectively: cirrhosis/class B Child, therapeutic schedule including Sofosbuvir without Ribavirin, liver stiffness values, male gender and presence of diabetes. A multivariate analysis performed on Child A cirrhotic patients, showed that Sofosbuvir based therapeutic treatment without Ribavirin had a HCC occurrence 5.7 higher than Ribavirin-based schedules with or without Sofosbuvir (p < 0.0001, OR: 5.686, 95% CI 2.455-13.169).
CONCLUSIONS
Our data suggest that early HCC occurrence appears more frequently related to Sofosbuvir-based therapy without Ribavirin which, indeed, seems to play a protective role on HCC onset. Therefore, a careful follow-up should be mandatory, especially in those regimens including Sofosbuvir without Ribavirin.
Identifiants
pubmed: 31462268
doi: 10.1186/s12967-019-2033-x
pii: 10.1186/s12967-019-2033-x
pmc: PMC6712712
doi:
Substances chimiques
Antiviral Agents
0
Types de publication
Journal Article
Multicenter Study
Research Support, Non-U.S. Gov't
Langues
eng
Sous-ensembles de citation
IM
Pagination
292Références
Liver Transpl. 2005 Sep;11(9):1086-92
pubmed: 16123959
Gut. 2006 Sep;55(9):1370-1
pubmed: 16905711
Nat Rev Cancer. 2006 Sep;6(9):674-87
pubmed: 16929323
Scand J Gastroenterol. 2010;45(2):250-5
pubmed: 19968615
Semin Liver Dis. 2010 Feb;30(1):61-74
pubmed: 20175034
J Hepatol. 2012 Apr;56(4):908-43
pubmed: 22424438
Gastroenterology. 2012 May;142(6):1274-8
pubmed: 22537433
Immunology. 2012 Nov;137(3):259-70
pubmed: 22891772
J Hepatol. 2015 Jul;63(1):199-236
pubmed: 25911336
J Hepatol. 2015 Apr;62(1 Suppl):S87-99
pubmed: 25920094
Hepatology. 2016 Jul;64(1):130-7
pubmed: 26946190
J Hepatol. 2016 Oct;65(4):719-726
pubmed: 27084592
BMC Surg. 2016 Apr 19;16:22
pubmed: 27094483
Ann Oncol. 2016 Aug;27(8):1467-74
pubmed: 27226385
J Hepatol. 2016 Oct;65(4):856-858
pubmed: 27318327
J Hepatol. 2016 Oct;65(4):727-733
pubmed: 27349488
Antimicrob Agents Chemother. 2016 Nov 21;60(12):7077-7085
pubmed: 27645237
Gastroenterol Hepatol (N Y). 2016 Dec;12(12):776-779
pubmed: 28035203
Antiviral Res. 2017 Jul;143:151-161
pubmed: 28412183
Hepatol Int. 2017 Jul;11(4):374-383
pubmed: 28643186
Cell Death Dis. 2017 Aug 24;8(8):e3017
pubmed: 28837142
Antiviral Res. 2017 Oct;146:139-145
pubmed: 28844749
Cell Immunol. 2018 Apr;326:52-59
pubmed: 28860007
Gastroenterol Hepatol (N Y). 2017 Jul;13(7):421-425
pubmed: 28867970
Gastroenterology. 2018 Feb;154(3):515-517.e3
pubmed: 29102620
J Biochem Mol Toxicol. 2018 Jan;32(1):null
pubmed: 29112301
J Hepatol. 2018 Aug;69(2):345-352
pubmed: 29551707
Hepatology. 2018 Sep;68(3):1010-1024
pubmed: 29604220
Gastroenterology. 2018 Aug;155(2):411-421.e4
pubmed: 29655836
Am J Gastroenterol. 2018 Aug;113(8):1251
pubmed: 29686274
Gastroenterology. 2018 Nov;155(5):1436-1450.e6
pubmed: 30031138