BACKGROUND: HIV reservoirs represent the major obstacles for eradication and are defined as a cell type that allows persistence of replication-competent HIV in patients on optimal long-term antiretroviral therapy (HAART). Several pilot clinical trials have been implemented to assess the value of experimental therapy to reduce reservoir size or eradicate HIV. In order to eradicate HIV, valproic acid was used as a new strategy to increase viral gene expression in the nucleus of infected cells with the expectation of generating a direct cell death or destruction by nearby cytotoxic cells. Previous pilot studies using VPA have showed conflicting results on the ability of VPA to reduce the size of HIV reservoirs. PURPOSE: As the role of VPA on HIV reservoirs remains unclear, we conducted a multicenter clinical trial with a specific study design to obtain optimal information on reservoir changes while exposing the smallest number of individuals to the experimental medication. METHOD: To this aim, a randomized, crossover design with 2 different treatment durations was implemented. By doubling the therapeutic period in one study arm, we were in a position to assess the impact of an extended duration of VPA on the size of the HIV reservoir and to evaluate the duration of treatment effects upon VPA withdrawal in the other arm. However, limitations for this type of study design included the logistical complexity of 2 uneven study arms and longer study duration. CONCLUSION: Despite the absence of demonstrable impact of VPA on reservoir size, such crossover study design should be considered in the early stage testing of novel HIV therapeutics targeted to reduce reservoir size or eradicate HIV.
RCT Entities:
BACKGROUND:HIV reservoirs represent the major obstacles for eradication and are defined as a cell type that allows persistence of replication-competent HIV in patients on optimal long-term antiretroviral therapy (HAART). Several pilot clinical trials have been implemented to assess the value of experimental therapy to reduce reservoir size or eradicate HIV. In order to eradicate HIV, valproic acid was used as a new strategy to increase viral gene expression in the nucleus of infected cells with the expectation of generating a direct cell death or destruction by nearby cytotoxic cells. Previous pilot studies using VPA have showed conflicting results on the ability of VPA to reduce the size of HIV reservoirs. PURPOSE: As the role of VPA on HIV reservoirs remains unclear, we conducted a multicenter clinical trial with a specific study design to obtain optimal information on reservoir changes while exposing the smallest number of individuals to the experimental medication. METHOD: To this aim, a randomized, crossover design with 2 different treatment durations was implemented. By doubling the therapeutic period in one study arm, we were in a position to assess the impact of an extended duration of VPA on the size of the HIV reservoir and to evaluate the duration of treatment effects upon VPA withdrawal in the other arm. However, limitations for this type of study design included the logistical complexity of 2 uneven study arms and longer study duration. CONCLUSION: Despite the absence of demonstrable impact of VPA on reservoir size, such crossover study design should be considered in the early stage testing of novel HIV therapeutics targeted to reduce reservoir size or eradicate HIV.
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Authors: Jesper D Gunst; Marie H Pahus; Miriam Rosás-Umbert; I-Na Lu; Thomas Benfield; Henrik Nielsen; Isik S Johansen; Rajesh Mohey; Lars Østergaard; Vibeke Klastrup; Maryam Khan; Mariane H Schleimann; Rikke Olesen; Henrik Støvring; Paul W Denton; Natalie N Kinloch; Dennis C Copertino; Adam R Ward; Winiffer D Conce Alberto; Silke D Nielsen; Maria C Puertas; Victor Ramos; Jacqueline D Reeves; Christos J Petropoulos; Javier Martinez-Picado; Zabrina L Brumme; R Brad Jones; Julie Fox; Martin Tolstrup; Michel C Nussenzweig; Marina Caskey; Sarah Fidler; Ole S Søgaard Journal: Nat Med Date: 2022-10-17 Impact factor: 87.241
Authors: Kateřina Trejbalová; Denisa Kovářová; Jana Blažková; Ladislav Machala; David Jilich; Jan Weber; Dana Kučerová; Ondřej Vencálek; Ivan Hirsch; Jiří Hejnar Journal: Clin Epigenetics Date: 2016-02-19 Impact factor: 6.551