HIV Clinical Trial
Official title:
A Phase III, Double Blind, Mulit-centre, Randomised Placebo Controlled, Pilot Study to Assess the Feasibility of Switching Individuals Receiving Efavirez With Continuing Central Nervous System (CNS) Toxicity to TMC125.
The purpose of the study is to examine the effect of switching from an antiretroviral
combination that includes efavirenz (Susitiva®), in individuals experiencing
efavirenz-related side effects, and replacing this with an investigational HIV medication
called Etravirine (TMC125).
The study will primarily investigate the effect of change in medication on your viral load
(the levels of the HIV virus in your blood), on immunological parameters (CD4 count), on
other safety parameters (such as cholesterol) your side effects and also on your quality of
life.
The majority of individuals who commence treatment for HIV in the UK start with a regimen
that includes EFV in combination with other antiretrovirals. These regimens are convenient
(once daily dosing) and highly efficacious. However EFV has several potential drawbacks
including continued CNS toxicity, the potential for teratogenesis and a low barrier to the
development of virological resistance. In the past the only alternative NNRTI available was
nevirapine which appears to have a lower rate of virological success and is associated with
potentially life threatening toxicities including hepatotoxicity and cutaneous toxicity
including the Stevens-Johnson syndrome.
Clinically controlled trials frequently reported undesirable nervous system side effects in
patients receiving 600 mg EFV with other antiretroviral agents, including
dizziness,insomnia, somnolence, impaired concentration and abnormal dreaming. CNS symptoms
of moderate to severe intensity were experienced by 19.4% of patients compared to 9.0% of
patients receiving control regimens. These symptoms were severe in 2.0% of patients
receiving EFV 600 mg daily and in 1.3% of patients receiving control regimens. In clinical
studies 2.1% of patients treated with 600 mg of EFV discontinued therapy because of nervous
system symptoms.
Nervous system symptoms usually begin during the first one or two days of therapy and often
resolve after the first 2 -4 weeks. However in a significant proportion of individuals it
continues with an adverse effect on quality of life. CNS toxicity may also worsen drug
compliance. In a study of uninfected volunteers, a representative nervous system symptom had
a median time to onset of 1 hour post dose and a median duration of 3 hours.
Nervous system symptoms may occur more frequently when EFV is taken concomitantly with meals
possibly due to increased EFV plasma. Dosing at bedtime seems to improve the tolerability of
these symptoms and can be recommended during the first weeks of therapy and in patients who
continue to experience symptoms although this is not always successful and may be associated
with vivid or disturbing dreams. Dose reduction or splitting the daily dose has not been
shown to provide benefit.
Other adverse events associated with efavirenz include rash (5-26%, usually minor),increased
cholesterol (20-40%) and triglycerides (6-11%), diarrhea (3-14%), nausea and hyperglycemia
(2-5%). Serious psychiatric adverse events such as precipitation of psychosis, seizure,
suicidal ideation, paranoia, mania and aggression have also been associated with use. These
are seen in <1% taking EFV and are thought to be more likely in those with a history of
mental illness/drug abuse or predisposition to psychological reactions.
TMC125 is a diarylpyrimidine derivative that has proven efficacy against HIV-1 including
activity in viral isolates with existing NNRTI signature mutations. Resistance to TMC125
also appears to develop less readily than to EFV and NVP. This has been attributed to its
molecular structure. TMC125 has demonstrated safety and efficacy in short term studies in
both treatment-naïve and NNRTI-resistant HIV-1 infected patients.
Recently published results from phase 3 trials give further support to these findings with
efficacy in reduction of HIV-1-RNA levels seen in patients with substantial NNRTI and PI
resistance when treated with TMC125 plus an optimized background.
TMC-125 is generally well tolerated and in particular has lower reported rates of CNS
toxicity than EFV. Animal studies have shown a low risk of teratogenesis. The major toxicity
of TMC125 has been skin rash which is usually self-limiting. In the repeated dose trials the
adverse events (AEs) reported in more than 10% of all subjects were headache, somnolence,
diarrhea, flatulence, nausea and vomiting, fatigue, fever, rash,and pruritus. Overall, AEs
were mild to moderate in intensity, with no apparent doseresponse relationship. No
consistent or clinically relevant changes in electrocardiogram (ECG) or vital signs were
observed with single and repeated TMC125 dosing.
TMC125 is a new NNRTI with proven efficacy against HIV-1 with several potential advantages
over EFV including no CNS toxicity and a high barrier to the development of resistance. This
study aims to investigate whether substitution of EFV with TMC125 leads to improvement of
CNS toxicity with continued virological suppression and immunological reconstitution and
whether this is associated with an improvement in quality of life.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Double Blind (Subject, Caregiver, Investigator), Primary Purpose: Treatment
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