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2028-08-30
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- INI - Artigos de Periódicos [3466]
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EFFICACY AND SAFETY OF RILPIVIRINE IN TREATMENT-NAIVE, HIV-1-INFECTED PATIENTS WITH HEPATITIS B VIRUS/HEPATITIS C VIRUS COINFECTION ENROLLED IN THE PHASE III RANDOMIZED, DOUBLE-BLIND ECHO AND THRIVE TRIALS
Efavirenz
Hepatitis
Hepatic safety
Non-nucleoside reverse transcriptase inhibitors
HBV
HCV
Author
Affilliation
Chelsea and Westminster Hospital/St Stephen's Centre. London, UK.
Centro Médico Puerta de Hierro/Universidad de Guadalajara. Departamento de Enfermedades Infecciosas. Jalisco, México.
Saint-Pierre University Hospital. Clinic of Infectious Diseases. Brussels, Belgium.
Centro Médico São Francisco. Curitiba, Brasil.
University of Miami. Division of Infectious Diseases. Miami, FL, USA.
Clinique Medicale du Quartier Latin. Montreal, Canada.
Beijing PUMC Hospital. Beijing, China.
University of Pennsylvania Hospital. Division of Infectious Diseases. Philadelphia, PA, USA.
Janssen Infectious Diseases BVBA. Beerse, Belgium.
Janssen Infectious Diseases BVBA. Beerse, Belgium.
Janssen Infectious Diseases BVBA. Beerse, Belgium.
Janssen Research & Development LLC. Titusville, NJ, USA.
Centro Médico Puerta de Hierro/Universidad de Guadalajara. Departamento de Enfermedades Infecciosas. Jalisco, México.
Saint-Pierre University Hospital. Clinic of Infectious Diseases. Brussels, Belgium.
Centro Médico São Francisco. Curitiba, Brasil.
University of Miami. Division of Infectious Diseases. Miami, FL, USA.
Clinique Medicale du Quartier Latin. Montreal, Canada.
Beijing PUMC Hospital. Beijing, China.
University of Pennsylvania Hospital. Division of Infectious Diseases. Philadelphia, PA, USA.
Janssen Infectious Diseases BVBA. Beerse, Belgium.
Janssen Infectious Diseases BVBA. Beerse, Belgium.
Janssen Infectious Diseases BVBA. Beerse, Belgium.
Janssen Research & Development LLC. Titusville, NJ, USA.
Abstract
OBJECTIVES:
The efficacy and hepatic safety of the non-nucleoside reverse transcriptase inhibitors rilpivirine (TMC278) and efavirenz were compared in treatment-naive, HIV-infected adults with concurrent hepatitis B virus (HBV) and/or hepatitis C virus (HCV) infection in the pooled week 48 analysis of the Phase III, double-blind, randomized ECHO (NCT00540449) and THRIVE (NCT00543725) trials.
METHODS:
Patients received 25 mg of rilpivirine once daily or 600 mg of efavirenz once daily, plus two nucleoside/nucleotide reverse transcriptase inhibitors. At screening, patients had alanine aminotransferase/aspartate aminotransferase levels ≤5× the upper limit of normal. HBV and HCV status was determined at baseline by HBV surface antigen, HCV antibody and HCV RNA testing.
RESULTS:
HBV/HCV coinfection status was known for 670 patients in the rilpivirine group and 665 in the efavirenz group. At baseline, 49 rilpivirine and 63 efavirenz patients [112/1335 (8.4%)] were coinfected with either HBV [55/1357 (4.1%)] or HCV [57/1333 (4.3%)]. The safety analysis included all available data, including beyond week 48. Eight patients seroconverted during the study (rilpivirine: five; efavirenz: three). A higher proportion of patients achieved viral load <50 copies/mL (intent to treat, time to loss of virological response) in the subgroup without HBV/HCV coinfection (rilpivirine: 85.0%; efavirenz: 82.6%) than in the coinfected subgroup (rilpivirine: 73.5%; efavirenz: 79.4%) (rilpivirine, P = 0.04 and efavirenz, P = 0.49, Fisher's exact test). The incidence of hepatic adverse events (AEs) was low in both groups in the overall population (rilpivirine: 5.5% versus efavirenz: 6.6%) and was higher in HBV/HCV-coinfected patients than in those not coinfected (26.7% versus 4.1%, respectively).
CONCLUSIONS:
Hepatic AEs were more common and response rates lower in HBV/HCV-coinfected patients treated with rilpivirine or efavirenz than in those who were not coinfected.
Keywords
TMC278Efavirenz
Hepatitis
Hepatic safety
Non-nucleoside reverse transcriptase inhibitors
HBV
HCV
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