Should Expectations about the Rate of New Antiretroviral Drug Development Impact the Timing of HIV Treatment Initiation and Expectations about Treatment Benefits?
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2014Metadata
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Khademi, Amin
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Should Expectations about the Rate of New Antiretroviral Drug Development Impact the Timing of HIV Treatment Initiation and Expectations about Treatment Benefits?
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Abstract
Background: Many analyses of HIV treatment decisions assume a fixed formulary of HIV drugs. However, new drugs are
approved nearly twice a year, and the rate of availability of new drugs may affect treatment decisions, particularly when to
initiate antiretroviral therapy (ART).
Objectives: To determine the impact of considering the availability of new drugs on the optimal initiation criteria for ART
and outcomes in patients with HIV/AIDS.
Methods: We enhanced a previously described simulation model of the optimal time to initiate ART to incorporate the rate
of availability of new antiviral drugs. We assumed that the future rate of availability of new drugs would be similar to the
past rate of availability of new drugs, and we estimated the past rate by fitting a statistical model to actual HIV drug
approval data from 1982–2010. We then tested whether or not the future availability of new drugs affected the modelpredicted
optimal time to initiate ART based on clinical outcomes, considering treatment initiation thresholds of 200, 350,
and 500 cells/mm3. We also quantified the impact of the future availability of new drugs on life expectancy (LE) and qualityadjusted
life expectancy (QALE).
Results: In base case analysis, considering the availability of new drugs raised the optimal starting CD4 threshold for most
patients to 500 cells/mm3. The predicted gains in outcomes due to availability of pipeline drugs were generally small (less
than 1%), but for young patients with a high viral load could add as much as a 4.9% (1.73 years) increase in LE and a 8%
(2.43 QALY) increase in QALE, because these patients were particularly likely to exhaust currently available ART regimens
before they died. In sensitivity analysis, increasing the rate of availability of new drugs did not substantially alter the results.
Lowering the toxicity of future ART drugs had greater potential to increase benefit for many patient groups, increasing
QALE by as much as 10%.
Conclusions: The future availability of new ART drugs without lower toxicity raises optimal treatment initiation for most
patients, and improves clinical outcomes, especially for younger patients with higher viral loads. Reductions in toxicity of
future ART drugs could impact optimal treatment initiation and improve clinical outcomes for all HIV patients.
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This work was partially supported by: R01AA017385-01 "A computer simulation of the Sub-Saharan HIV pandemic that can estimate benefit and value
from alcohol interventions" - PI: Braithwaite (http://www.niaaa.nih.gov/), and U24AA022007-01 "The Operations Research Collaboration for Alcohol Abuse and
Aids - ORCAAA" -PI: Braithwaite (http://www.niaaa.nih.gov/) and NS grant (NS F CMMI-0546960). The funders had no role in study design, data collection
and analysis, decision to publish, or preparation of the manuscript.
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URI: https://repositorio.uchile.cl/handle/2250/126801
DOI: doi:10.1371/journal.pone.0098354
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Plos One 9(6): e98354. 2014
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