HIV Clinical Trial
Official title:
Effect of Rifampin-containing Anti-TB Treatment on Efavirenz Pharmacokinetics in HIV/TB Co-infected Children Aged 3 - 14 Years
Efavirenz is an essential component of HIV treatment in children aged 3 years or older on anti-tuberculosis (anti-TB) treatment. However, the appropriate efavirenz dose during anti-TB treatment remains unclear. Rifampin (an anti-TB drug) increases the activity of the drug metabolizing enzymes that breakdown efavirenz, which may lead to low blood levels of efavirenz and treatment failure during cotreatment. The drug-to-drug interactions between the HIV and anti-TB drugs also vary between individuals based on genetic factors. This study will investigate the effects of anti-TB treatment, as well as drug-gene interactions on the blood concentrations of efavirenz in children with HIV and TB infections. Such data could enhance optimization of efavirenz dosage or selection of alternate regimens in some children.
Efavirenz-based antiretroviral therapy (ART) is the preferred regimen in children older than
3 years on rifampin-containing anti-TB therapy. Efavirenz trough plasma concentrations below
1000 ng/mL have been associated with increased risk of virologic failure among HIV-infected
adults, while concentrations above 4000 ng/mL have been associated with risk of central
nervous system side effects. Efavirenz is primarily metabolized by hepatic CYP2B6, with
secondary contributions from CYP2A6. On average, rifampin co-administration causes a 26%
reduction in efavirenz plasma exposure but some individuals have paradoxically elevated
efavirenz concentrations with co-administration in adult pharmacokinetic studies. The
inter-individual variability in the drug-to-drug interactions suggest that efavirenz dose
adjustment with concomitant anti-TB therapy may not be necessary in some patients. In
children, there is very limited data on the pharmacokinetic interactions between
rifampin-containing TB treatment and efavirenz. To our knowledge, there is only one
published study in children to date. Among 15 TB/HIV co-infected children treated with
standard efavirenz-based active antiretroviral therapy and rifampin-containing TB treatment,
a wide inter-patient variability in efavirenz concentration as well as a bimodal
distribution of efavirenz trough concentrations were observed. Overall, rifampin-containing
anti-TB treatment had no significant influence on the mean change in efavirenz concentration
in the study population as a whole, but 60% and 53% of children had efavirenz trough
concentration < 1000 ng/mL during and after anti-TB, respectively. This data suggest that
current dosing of efavirenz may be suboptimal in a large proportion of children irrespective
of anti-TB therapy. To overcome the risk of under-dosing of efavirenz especially with
concurrent anti-TB treatment, the WHO recommended prescribing the maximum dose for each
weight-band when efavirenz is coadministered with anti-TB treatment. This study seeks to
evaluate whether the current dosing of efavirenz provides adequate efavirenz concentrations
in children, as well as explore how genetic factors influence efavirenz pharmacokinetics
with concomitant anti-TB treatment. The specific hypotheses to be tested are:
1. At the population level, efavirenz plasma concentrations in TB/HIV co-infected children
who are treated with the maximized weight-based efavirenz dosage during
rifampin-containing anti-TB therapy will be comparable to concentrations in
HIV-infected children receiving ART without anti-TB treatment.
2. Co-treatment with rifampin- and efavirenz-containing therapies will lead to
substantially decreased (by at least 40%) efavirenz concentration in the children with
CYP2B6 extensive but not in those with intermediate or slow metabolizer genotypes.
A two-arm, as well as a two-period pharmacokinetic study in HIV-infected children with and
without TB will be performed at the Komfo Anokye Teaching Hospital (KATH), Kumasi, Ghana.
Eligible participants will include children aged 3 - 14 years with HIV with or without TB
coinfection, ART-naïve and eligible to initiate ART. The ART regimen will consist of the WHO
recommended weight-band dosing of efavirenz (10-13.9kg - 200 mg; 14-24.9kg - 300mg;
25-39.9kg - 400 mg and > 40Kg - 600 mg), plus ZDV 180 - 240 mg/m2 and 3TC 4 mg/kg twice
daily. Tenofovir may be used in place of ZDV. Standard anti-TB therapy will be prescribed to
the co-infected patients and will start immediately upon TB diagnosis.
A complete medical history, physical examination, and staging of HIV disease will be
performed before initiation of ART. Baseline measurements prior to initiation of ART will
include CBC, blood urea nitrogen, creatinine, LFTs, CD4 cell count determination and plasma
HIV-1 RNA level. Weeks 12 and 24 CD4 cell count and plasma HIV-1 RNA will obtained at
scheduled follow-up. Pharmacokinetic sampling will be performed at week 4 of ART in both
arms and at 4 weeks after anti-TB treatment in the co-infected group. At each sampling time,
3 mL of blood will be collected into an EDTA tube. Blood samples will be collected at times
0 2, 8, 12 and 24 hours post-dose for determination of efavirenz concentrations. Efavirenz
concentrations in plasma will be measured using a HPLC-MS. After sample analysis, a data set
will be constructed. Anticipated covariates included in this data set to be explored will
include age, sex, weight, relevant drug-metabolizing enzyme genotype, TB therapy status
(on/off), and CD4 cell count. Nonlinear mixed-effects modeling (using NONMEM, version VI)
will be used to estimate pharmacokinetic parameters (CL/F, V/F, AUC, Cmin, Cmax, elimination
rate constant), inter-individual error, and residual error. Results of this population
analysis may be used to simulate alternative efavirenz dosing strategies in this TB/HIV
co-infected population, or in relevant sub-populations with variant PK/pharmacogenetics.
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