HIV Drug Resistance Clinical Trial
Official title:
Impact of HIV Drug Resistance Testing, and Subsequent Change to an Individualized Therapy Based on the Resistance Profile, in Children, Adolescents and Adults With Virological Failure of Their HIV Therapy, in Three HIV Clinics in Tanzania
The current therapy regimens in Sub-Saharan countries, consisting of standardized first and
second line drug combinations, yield a high rate of treatment failure, even within the first
12 months of therapy (23). These and other facts hint at the need for HIV resistance testing
to improve treatment outcomes in resource-limited settings, but no prospective clinical data
about this intervention exists. The proposed study aims to evaluate the impact of HIV drug
resistance testing, and subsequent change to an individualized (second-line) therapy based on
the resistance profile, in Tanzanian patients (children, adolescents and adults) with
virological failure of their first-line and second-line therapy. Additionally, prevalence,
patterns and clinical impact of HIVDR will be assessed, as well as the effect of enhanced
adherence counselling.
The results of this study will help doctors to take evidence-based diagnostic and therapeutic
decisions at an individual level, and will inform policy-makers in their decisions about
future treatment and management concepts for HIV/AIDS.
HIV/AIDS is one of the main health challenges of our time, with a global burden of disease
higher than any other infectious disease. The widespread use of antiretroviral drugs has
changed its face from a fatal fate to a chronic disease. However, there are still many
differences in the standard of care globally. Drug resistance testing is routinely performed
in high income countries, but is often not available in resource limited settings. Instead,
treatment consists of standardized therapy regimes, chosen from a limited amount of
antiretroviral drugs. This may contribute to the high rates of virological failure seen in
patients, and especially children and adolescents, on therapy. Virological failure persisting
despite intensified enhanced adherence-counselling result in poor treatment success in HIV
infected adults, children and adolescents on treatment and therefore early deaths. If therapy
failure occurs, and HIV drug resistance is the likely reason, physician in Tanzania need to
blindly choose a second-line therapy regimen, without knowledge of the exact resistance
profile. However, multiple studies have discovered high rates of HIV drug resistance in
patients with first line treatment failure, and even in therapy-naïve patients. To obtain
information about presence of resistance mutations HIV genotypic resistance testing is
required. This test is used to detect HIV genomic mutations that confer resistance to
specific types of antiretroviral drugs as an aid in monitoring and treating HIV-infection.
The test identifies mutation on the protease and reverse transcriptase gene, which are
responsible for very crucial steps in the viral replication process. Results from this test
can identify the medication for whom the virus is still susceptible and for whom it is
already resistant. With this, it can be avoid switching to second-line regimen without the
knowledge of the presence or absence of antiretroviral drug resistance. An individualized
therapy can follow making sure that medication works best and the clinical outcome can
increase.
While the positive impact of HIV resistance testing on treatment outcomes in high-income
countries is well established, no prospective data has been published about the effect in
resource-limited settings. This absence of data poses a hole in clinical knowledge, because
the results from high-income countries are not readily transferable to low-income settings.
The proposed study aims to evaluate the impact of HIV drug resistance testing, and subsequent
change to an individualized (second-line) therapy based on the resistance profile, compared
to standardized second-line therapy. The study is designed as a randomised controlled trial.
The study participants, Tanzanian patients (children, adolescents and adults) with
virological failure of their first-line therapy, will be recruited at several study sites.
All patients will first receive enhanced adherence counselling. The patients that still show
virological failure three months after the counselling will be eligible for resistance
testing. The regimen will be switched to individualized (second-line) ART or standardized
second-line ART, and clinical, immunological and virological outcome parameters will be
collected in a 6 month and 12 month follow up visit (Group I,II,III IV). In addition to the
outcome of individualized therapy, the proposed study would yield insights about the
prevalence and patterns of HIV drug resistance in patients with failure of their first-line
therapy, and also about the effectiveness of enhanced adherence counselling.
For ethical reasons also 250 seconnd line treatment failure patients (Group V) with fast
clinical progress will be included and transfered directly to the individualized therapy arm.
With that we hope to bring them back to a working treatment.
The main diagnostic method of this study, HIV genomic sequencing, will be implemented and
performed at the National Institute for Medical Research in Mwanza, Tanzania. This will
contribute directly to the HIV-related diagnostic capacities of Tanzanian laboratories.
;
| Status | Clinical Trial | Phase | |
|---|---|---|---|
| Recruiting |
NCT02507921 -
Resistance in HIV+ in North and South
|
N/A | |
| Withdrawn |
NCT03928834 -
Sustainable Adherence and Prevention of HIV Drug Resistance in Adolescents
|
N/A |