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Optimal Dosing of 1st Line Antituberculosis and Antiretroviral Drugs in Children (a Pharmacokinetic Study)

Information source: University of Cape Town
ClinicalTrials.gov processed this data on August 23, 2015
Link to the current ClinicalTrials.gov record.

Condition(s) targeted: Tuberculosis; HIV

Intervention: 8 hourly LPV/r during TB treatment (Drug); Nevirapine (Drug); Lopinavir/Ritonavir (Drug)

Phase: Phase 4

Status: Recruiting

Sponsored by: University of Cape Town

Official(s) and/or principal investigator(s):
Helen M McIlleron, PhD, Principal Investigator, Affiliation: University of Cape Town
Heather Zar, PhD, Principal Investigator, Affiliation: University of Cape Town

Overall contact:
Heln McIlleron, PhD, Phone: 27214066292, Email: helen.mcilleron@uct.ac.za

Summary

The aims of this project are to: 1. To evaluate the pharmacokinetics of first line antituberculosis drugs (isoniazid, rifampicin, pyrazinamide and ethambutol) when applying the 2010 WHO/IUATLD dosing guidelines across pediatric populations (0-12 years of age, HIV infected and uninfected, and with varied nutritional status) in Cape Town, South Africa and Blantyre, Malawi. 2. To evaluate an 8-hourly weight band-based dosing strategy for lopinavir/ritonavir using the commercially available lopinavir/ritonavir (4: 1 ratio) in children in South Africa receiving rifampicin-based antituberculosis treatment. 3. To evaluate the pharmacokinetics of nevirapine in children in Malawi receiving rifampicin-based antituberculosis treatment.

Clinical Details

Official title: Optimal Dosing of 1st Line Antituberculosis and Antiretroviral Drugs in Children (a Pharmacokinetic Study)

Study design: Allocation: Non-Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment

Primary outcome: Area under the concentration time curve (AUC) for rifampicin, isoniazid, pyrazinamide, ethambutol, lopinavir and nevirapine

Detailed description: HIV and tuberculosis are a major public health problem in children. Challenges to treat children with tuberculosis include a lack of knowledge about optimal dosing of first line antituberculosis drugs across ages, nutritional status and HIV infection status, the absence of an appropriate regimen to co-administer rifampin and lopinavir/ritonavir, the key first line drugs for tuberculosis and HIV, and uncertainty about NVP exposure in young children during rifampin-based tuberculosis therapy. In total, 240 children < 12 years of age with tuberculosis will be enrolled at Red Cross Children's Hospital in Cape Town and Queen Elizabeth Central Hospital, Blantyre. In the second month of antituberculosis treatment, one dose of the drugs in their first-line regimens will be administered according to 2010 WHO/IUATLD guidelines (study drugs) and blood will be sampled for pharmacokinetic analysis over the following 8-10 hours. Children on antiretroviral treatment (started prior to or during TB treatment) will receive 2 weeks of antiretrovirals (lopinavir/ritonavir or nevirapine) according in the study doses (adjusted 8 hourly doses of lopinavir/ritonavir, or nevirapine doses according to WHO's recommended weight band-based doses) in combination with antituberculosis treatment, prior to pharmacokinetic assessments of both antiretroviral and antituberculosis drugs. Children receiving nevirapine will also undergo pharmacokinetic evaluation 1 month after completion of antituberculosis treatment to evaluate nevirapine concentrations in the absence of antituberculosis drugs. In addition to the 240 children with tuberculosis, 25 HIV infected South African children without tuberculosis will be recruited to evaluate lopinavir concentrations in the absence of antituberculosis drugs. A population approach will be used to estimate the optimal doses of rifampicin, isoniazid, pyrazinamide and ethambutol in children according to covariates (e. g. age, weight, HIV status, nutritional status) found to have an important influence on the drug concentrations. Similarly population models will be used to describe lopinavir/ritonavir and nevirapine pharmacokinetics in children receiving rifampicin-based antituberculosis treatment, evaluate the dosing approaches and to simulate alternative optimal dosing approaches as indicated.

Eligibility

Minimum age: 1 Month. Maximum age: 12 Years. Gender(s): Both.

Criteria:

Inclusion Criteria: ALL STUDY PARTICIPANTS

- Aged < 12 years.

- Weighing > 1. 5 kg and < 30 kg.

- Written informed permission of parent or legal guardian for their child to

participate.

- Absence of clear indication of unwillingness or refusal to participate, and in

children > 7 years of age, assent to participate.

- No contraindications to PK sampling (children with obviously very poor venous access

will not be included).

- Able to comply with study visits and procedures including regular adherence to

routine medication, and adherence to the study medication.

- Enrollment will be deferred in children with acute severe illness which would likely

jeopardize participation (such as illness causing severe respiratory impairment, acute severe diarrhea, acute central nervous system impairment, severe life threatening systemic illness, or other severe conditions requiring hospitalization which would jeopardize participation). Children may be enrolled after recovery from acute illness. ADDITIONAL CRITERIA FOR THE MAIN TB COHORT AND SUBSTUDIES 1. Main TB cohort INCLUSION A recent diagnosis of TB and receiving intensive phase antiTB treatment with 1st-line drugs (rifampicin, isoniazid, pyrazinamide with or without ethambutol, in standard doses). 2. LPV SUBSTUDY CASES & CONTROLS

- Children in whom ART with a LPV/r-containing regimen is indicated, OR, Children

established on a LPV/r-containing regimen.

- ALT < 5-times the upper limit of the normal range.

- Children weighing 3. 0 - 19. 9 kg.

- Neonates must have a postmenstrual age of at least 42 weeks and a postnatal age

of at least 14 days. CASES

- HIV infected children enrolled to the main cohort with at least 2 weeks remaining

before the end of intensive phase antiTB treatment such that PK sampling can be scheduled after 2 weeks of combined ART and antiTB treatment, but before the continuation phase of antiTB treatment is started. CONTROLS

- HIV infected children without TB.

Weighted enrollment of controls will be performed such that the number of controls in each of the age groups < 6 months, 6 months to 2 years, and > 2 years, will be approximately equal to the numbers of cases in those age groups. As most of the children with TB will be started on ART after their TB diagnosis, recruitment of controls will be focused on children who have recently started ART (on treatment < 3 months). 3. NVP SUBSTUDY

- HIV infected children receiving intensive phase antiTB treatment and enrolled to

the main study cohort

- Started on ART including NVP (in WHO's recommended weight band-based doses) and

2 nucleoside reverse transcriptase inhibitors. Exclusion Criteria:

- Indication for increased or reduced doses of 1st-line antiTB drugs (e. g. marked

hepatic or renal impairment, TB meningitis).

Locations and Contacts

Heln McIlleron, PhD, Phone: 27214066292, Email: helen.mcilleron@uct.ac.za

Queen Elizabeth Central Hospital, Blantyre, Malawi; Recruiting
Carmen Gonzalez, MD, MSc, Phone: 0026 5991416730, Email: Gonzalez@liverpool.ac.uk
Gerraint Davies, PhD, Principal Investigator

Desmond Tutu Centre, Cape Town, Western Cape, South Africa; Recruiting
Adrie Bekker, MMed, Phone: 27219389198, Email: adrie@sun.ac.za
Anneke Catharina Hesseling, PhD, Principal Investigator

Red Cross Childrens Hospital, Cape Town, Western Cape 7700, South Africa; Recruiting
Heather ZAR, PhD, Phone: 27216585350, Email: heather.zar@uct.ac.za
Margaretha Prins, Phone: 27216863163, Email: margaretha.prins@uct.ac.za
Heather ZAR, PhD, Principal Investigator

Additional Information

Starting date: November 2012
Last updated: December 2, 2014

Page last updated: August 23, 2015

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