HIV Clinical Trial
Official title:
Phase IV, Two-arm, Open-label, Single-centre Randomised Pilot Study to Assess the Feasibility of Immediate or Deferred Switching of HIV-infected Individuals Intolerant of Efavirenz, Ritonavir-boosted Lopinavir or Ritonavir-boosted Darunavir
The purpose of the study is to examine the effects of switching from antiretroviral
combinations that includes efavirenz (Sustiva®), lopinavir/ritonavir (Kaletra®) or
atazanavir/ritonavir (Reyataz®/Norvir®) in individuals experiencing side effects from one of
these agents, and replacing these with a new HIV medication called Darunavir also given with
ritonavir (Norvir®).
The study will primarily investigate the effect of change in medication on the subjects
viral load (the levels of the HIV virus in the blood), on immunological parameters (CD4
count) and on other safety parameters (such as cholesterol) and also quality of life.
The advent of highly active antiretroviral therapy (HAART) has revolutionised the treatment
of HIV disease, with both patients and physicians enjoying the marked reductions in HIV
related morbidity and mortality. However, as long term therapeutic success has become a
realistic goal of treatment, there are increasing reports of toxicities associated with
therapy.
Indeed since the advent of HAART the major reason for change in therapy has not been a lack
of efficacy associated with drug regimens but the toxicity associated with individual
agents. Although the potential adverse events associated with antiretrovirals are manifold
there are signature treatment-limiting toxicities associated with particular agents such as
EFV and CNS/neuropsychiatric adverse events, LPV/r and gastrointestinal toxicity and ATV/r
and jaundice.
A recent study performed at the Chelsea and Westminster hospital showed that 61% of regimen
switches were due to toxicity and the majority of these occurred after 12 weeks of therapy.
Darunavir is a recently licensed protease inhibitor which requires ritonavir
boosting.Currently DRV/r is licensed for use in treatment-experienced individuals. In
triple-class experienced patients ritonavir boosted darunavir has been associated with
greater viral load reductions when combined with optimized background (OB) than OB alone. A
study of PI experienced patients randomized to receive Kaletra or ritonavir boosted
darunavir with optimised background therapy showed significantly higher rates of virological
suppression in the DRV/r arm; rates of toxicities were similar overall but less diarrhoea in
the DRV/r than the Kaletra arm. Darunavir is licensed twice daily and has a high barrier to
the development of resistance. DRV/r dosed at 800/100mg once daily has been compared with
LPV/r in treatment-naïve subjects. DRV/r was non-inferior to LPV/r overall and performed
significantly better than LPV once daily and in subjects with a high baseline viral load.
DRV/r and LPV/r have also been compared head to head in 'early'treatment-experienced
patients (failing first or second line therapy but LPV-naive). Overall DRV/r exhibited
superiority to LPV/r with 77% and 67% achieving viral suppression to less than 50 copies/ml
by intent-to-treat analysis respectively (95% confidence interval for the difference 2-17%;
p <0.0001). Animal studies have shown a low risk of teratogenesis associated with DRV.
This study aims to investigate whether substitution of NNRTI/PI with ritonavir boosted
darunavir leads to resolution of toxicity associated with these drugs, continued virological
suppression and immunological reconstitution and whether this is associated with an
improvement in quality of life.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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