Desimplification to multi-tablet antiretroviral regimens in human immunodeficiency virus-type 1 infected adults: A cohort study

Maria C Rossi; Walter O Inojosa; Giuseppe Battistella; Antonella Carniato; Francesca Farina; Mario Giobbia; Rodolfo Fuser; Pier G Scotton

doi:10.12998/wjcc.v7.i14.1814

Desimplification to multi-tablet antiretroviral regimens in human immunodeficiency virus-type 1 infected adults: A cohort study

World J Clin Cases. 2019 Jul 26;7(14):1814-1824. doi: 10.12998/wjcc.v7.i14.1814.

Authors

Maria C Rossi¹, Walter O Inojosa², Giuseppe Battistella³, Antonella Carniato¹, Francesca Farina¹, Mario Giobbia¹, Rodolfo Fuser¹, Pier G Scotton¹

Affiliations

¹ Infectious Diseases Unit, Treviso Hospital, Treviso 31100, Italy.
² Infectious Diseases Unit, Treviso Hospital, Treviso 31100, Italy. walteromar.inojosa@aulss2.veneto.it.
³ Epidemiology and Statistic Unit, Azienda ULSS 2 "Marca Trevigiana", Treviso 31100, Italy.

Abstract

Background: Highly active antiretroviral therapy (HAART) is provided free of charge to all human immunodeficiency virus (HIV) positive residents in Italy. As fixed dose coformulations (FDCs) are often more expensive in comparison to the same drugs administered separately in a multi-tablet regimen (MTR), we considered a cost-effective strategy involving patients in the switch from their FDCs to corresponding MTRs including generic antiretrovirals.

Aim: To verify if this would affect the virological and immunological response in comparison to maintaining the FDC regimens.

Methods: From January 2012 to December 2013, we assessed the eligibility of all the HIV-1 positive adults on stable HAART being treated at our hospital-based outpatient clinic in Treviso, Italy. Participants who accepted to switch from their FDC regimen to the corresponding MTR joined the MTR group, while those who maintained a FDC regimen joined the FDC group. Clinical data, including changes in HAART regimens, respective reasons why and adverse effects, were recorded at baseline and at follow-up visits occurring at weeks 24, 48 and 96. All participants were assessed for virological and immunological responses at baseline and at weeks 24, 48 and 96.

Results: Two hundred and forty-three eligible HIV-1 adults on HAART were enrolled: 163 (67%) accepted to switch to a MTR, joining the MTR group, while 80 (33%) maintained their FDCs, joining the FDC group. In a parallel analysis, there were no significant differences in linear trend of distribution of HIV-RNA levels between the two groups and there were no significant odds in favour of a higher level of HIV-RNA in either group at any follow-up and on the overall three strata analysis. In a before-after analysis, both FDC and MTR groups presented no significant differences in distribution of HIV-RNA levels at either weeks 48 vs 24 and weeks 96 vs 24 cross tabulations. A steady increase of mean CD4 count was observed in the MTR group only, while in the FDC group we observed a slight decrease (-23 cells per mmc) between weeks 24 and 48.

Conclusion: Involving patients in the switch from their FDC regimens to the corresponding MTRs for economic reasons did not affect the effectiveness of antiretroviral therapy in terms of virological response and immunological recovery.

Keywords: Fixed dose coformulation regimens; Fixed-dose coformulations; Highly active antiretroviral therapy; Human immunodeficiency virus; Multitablet regimens.