Safety, Tolerability, Drug Interactions, and Antiviral Activity of Rilpivirine in Antiretroviral-Naive HIV-Infected Children Less Than 12 Years of Age



Status:Not yet recruiting
Conditions:HIV / AIDS, HIV / AIDS
Therapuetic Areas:Immunology / Infectious Diseases
Healthy:No
Age Range:2 - 11
Updated:2/8/2015
Start Date:September 2014

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A Phase I/II, Open-Label Trial to Evaluate the Safety, Tolerability, Pharmacokinetics and Antiviral Activity of Rilpivirine in Antiretroviral Naive HIV-1 Infected Children, < 12 Years of Age

Development of tolerable and effective antiretroviral (ARV) drugs for use in children and
adolescents remains a high priority. First-line therapy with non-nucleoside reverse
transcriptase inhibitors (NNRTIs) has proven to be effective for HIV-1-infected infants,
children, and adolescents. This study will evaluate the safety, effectiveness, and dosing
levels of the NNRTI rilpivirine (RPV) when given with two other ARV drugs in
treatment-naive, HIV-1-infected children less than 12 years of age.

This study will enroll HIV-1-infected children less than 12 years of age who are naive to
antiretroviral therapy (ART) (have never taken ARV drugs). Study participants will be
assigned to 1 of 2 cohorts based on age. Cohort 1 will include children at least 6 years of
age to less than 12 years of age. Cohort 2 will include children at least 2 years of age to
less than 6 years of age. Each cohort will consist of two stages: Stage 1 and Stage 2. Stage
1 will be the initial dose finding stage. Participants will begin treatment with daily RPV
and 2 nucleoside reverse transcriptase inhibitors (NRTIs). The 2 NRTIs will be selected by
the site investigator but will not be provided through the study. This stage of the study
will involve intense pharmacokinetic (PK) sampling to evaluate the safety, tolerability, and
antiviral activity of RPV, which will allow for the selection of an RPV dose to use in Stage
2 of the study. Participants in both cohorts will remain on RPV-based therapy for up to 48
weeks.

Study enrollment will begin with Cohort 1. Once data from Cohort 1 has been reviewed and an
RPV dose has been approved, enrollment for Cohort 2 will begin.

Study participation will include at least 12 study visits over 48 weeks. Participants who
complete 48 weeks of RPV treatment and are benefiting from the drug will continue on the
study and receive RPV as part of a long-term safety follow-up for a minimum of 4 additional
years. Study visits in this stage of the study will occur every 24 weeks.

At most visits, participants will give a medical history and undergo a physical exam, blood
collection, and urine collection. At some visits, participants will also undergo an
electrocardiogram (ECG), adrenocorticotropic hormone (ACTH) stimulation test (consisting of
blood collection and an injection of ACTH), and determination of the participant's stage of
sexual development.

Inclusion Criteria - Stage 1, Step 1 and Stage 2

- A confirmed HIV-1 infection. More information on this criterion can be found in the
protocol.

- Participant has never been treated with an HIV vaccine

- No evidence of prior ARV drug use with the exception of prior use of zidovudine (AZT)
for up to 6 weeks to prevent mother-to-child transmission

- HIV-1 plasma viral load (VL) at screening greater than 500 HIV-1 RNA copies/mL but
less than or equal to 100,000 HIV-1 RNA copies/mL (assayed by RNA polymerase chain
reaction [PCR] standard specimen procedure) Note: Participants may be re-screened
once only, if their baseline VL does not meet the entry criteria.

- In the judgment of the investigator, it is appropriate to initiate ARV therapy based
on the participant's medical condition and taking into account guidelines for the
treatment of HIV-1 infection in children

- Results from the genotypic resistance testing at screening demonstrate sensitivity to
the selected NRTIs for the chosen background regimen

- Able to swallow whole tablets (Cohort 1 initial dose only)

- Female participants who are of childbearing potential and who are engaging in sexual
activity that could lead to pregnancy, must use two adequate birth control methods
while on study and for 4 weeks after stopping study drug. More information on this
criterion can be found in the protocol.

Inclusion Criteria - Stage 1, Step 2

- Participants belonging to a cohort that failed Stage 1 Step 1 initial dose that meet
the following criteria (as determined by the study team): Are able to have an
adjustment in study drug dose (and the new dose would not exceed 25 mg) and appear to
have room to stay within therapeutic range on the new dose

Exclusion Criteria - Stage 1, Step 1 and Stage 2

- Having documented genotypic evidence of RPV resistance. More information on this
criterion can be found in the protocol.

- Documented evidence of infection during breastfeeding by a mother taking NNRTI-based
ART. If there are no data or no history available then the participant would be
eligible as long as all other inclusion and exclusion criteria are fulfilled.

- Documented evidence of maternal NNRTI use during pregnancy. If there are no data or
no history available then the participant would be eligible as long as all other
inclusion and exclusion criteria are fulfilled.

- Previously documented HIV-2 infection in participant or participant's mother. If
there are no data or no history available then the participant would be eligible as
long as all other inclusion and exclusion criteria are fulfilled.

- Use of disallowed medication from 4 weeks prior to the entry visit or anticipated use
of any disallowed medications

- A) Participant has used chronic systemic immunosuppressive agents within 30 days
prior to entry or is anticipated to need chronic systemic immunosuppressive agents
during the study. Short courses of systemic corticosteroids (e.g., prednisone or
equivalent up to 2 mg/kg/day for less than or equal to 7 days) are permitted, as long
as the use was greater than 30 days prior to entry; B) participant has used both
chronic inhaled and intranasal steroids within 30 days prior to entry. Use of either
inhaled or intranasal steroids are allowed.

- Participant has any active AIDS-defining illness (Category C conditions according to
the Centers for Disease Control and Prevention [CDC] revised Classification System
for HIV Infection 1994), within 30 days prior to screening. Stable not currently
active conditions that are not likely to interfere with safety assessments may be
allowed with permission from the protocol team.

- Any active clinically significant disease or findings (other than HIV infection)
during screening or medical history or physical examination that in the
investigator's opinion, would compromise the outcome of the study

- Any confirmed Grade 3 or 4 laboratory toxicity according to the Division of AIDS
(DAIDS) grading table at screening, except for: asymptomatic Grade 3 absolute
neutrophil count decrease; asymptomatic Grade 3 platelet count decrease; asymptomatic
Grade 3 total amylase, triglyceride, cholesterol elevation

- Participant has active tuberculosis and/or is being treated for tuberculosis at
screening

- Participant has one or more of the following risk factors for ECG QTc prolongation:

- A confirmed prolongation of QT/QTc interval, (e.g., repeated demonstration of
QTcF [Fridericia correction] interval greater than 450 ms in the screening ECG
(i.e., retesting to reassess eligibility will be allowed once using an
unscheduled visit during the screening period)

- Pathological Q-waves (defined as Q-wave greater than 40 ms or depth greater than
0.4-0.5 mV)

- Evidence of ventricular pre-excitation

- Electrocardiographic evidence of complete right or complete or incomplete left
bundle branch block

- Evidence of second or third degree heart block

- Intraventricular conduction delay with QRS duration greater than 120 ms

- Bradycardia as defined by sinus rate less than 50 bpm

- Personal or family history of long QT syndrome

- Personal history of cardiac disease, symptomatic or asymptomatic arrhythmias,
with the exception of sinus arrhythmia

- Syncopal episodes

- Risk factors for Torsade de Pointes (e.g., heart failure, hypokalemia)

- Participant's family is unlikely to adhere to the study procedures, keep
appointments, or is planning to relocate to a non-IMPAACT study site during the study

- Hepatitis B virus surface antigen (HBsAg) positive or hepatitis C virus (HCV)
antibody positive

- Any history of malignancy

- Participant enrolled in another clinical trial of an investigational agent or
experimental vaccine or a compound or device which is not commercially available

- Any history of adrenal insufficiency

- Pregnancy or breastfeeding if of childbearing potential
We found this trial at
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Aurora, Colorado 80045
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Seattle, Washington 98101
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