HIV Infections Clinical Trial
Official title:
Tenofovir Disoproxil Fumarate Salvage Therapy in HIV-Infected Children and a Study of Its Effect on Bone Metabolism
This study will examine the long-term effects, particularly on bone metabolism, of the drug
tenofovir DF in children with HIV infection. Tenofovir DF is approved for treating
HIV-infected adults, but its use in children has not yet been approved. The drug may be
helpful for children who have been treated with many other drugs and still have detectable
HIV in their blood despite ongoing therapy. In a previous study, many children given
tenofovir DF responded well, with increases in T-cell counts and decreases in viral load.
However, many children also experienced bone thinning. This study will explore the problem
of bone thinning in children taking tenofovir DF in combination with highly active
antiretroviral therapy (HAART).
HIV-infected patients from 4 to 20 years old who are taking tenofovir DF or for whom
tenofovir DF treatment has been recommended may be eligible for this 3-year study.
Participants take tenofovir DF every day in addition to their antiretroviral therapy. They
have frequent follow-up visits for tests and procedures as follows:
- Study days 0, 2, and 4: blood tests.
- Screening and every study visit starting day 6: Physical exam, medical history, blood
and urine tests.
- Baseline and every 48 weeks: Dental and eye examinations, kidney ultrasound, tuberculin
skin testing, chest x-ray, electrocardiogram and echocardiogram, computed tomography
(CT) scan, neuropsychological testing and neurologic assessment.
- The bone age hand x-rays are done every 24 weeks, unless the growth plates are fused
(i.e. the child has stopped growing)
- DEXAs are done at 0, 12, 24 weeks and every 24 weeks thereafter. Dual energy x-ray
absorptionometry (DEXA) scan is used to assess bone density. The patient lies still on
a table while the spine and hip are scanned using a small amount of radiation. Only the
spine and hip are scanned in the DEXA scan test.
- Baseline and week 24: Optional bone biopsy. Some patients are asked to undergo a bone
biopsy to better understand the effect of Tenofovir DF on bone. For the procedure, the
child is given a sedative. The skin over the hipbone is numbed with a small needle, a
small incision is made and a larger needle is inserted into the bone. Some of the bone
tissue is withdrawn through the needle and the incision is closed.
- Possible lumbar puncture (spinal tap): This optional procedure analyzes cerebrospinal
fluid (CSF), the fluid that bathes the brain and spinal cord. The patient is given a
local anesthetic and a needle is inserted into the space between the bones in the lower
back where the CSF circulates below the spinal cord. A small amount of fluid is
collected through the needle. There is no specific schedule for this procedure if the
patient opts for it.
Patients who are benefiting from tenofovir DF therapy but show signs of bone effects are
offered treatment with pamidronate (Aredia), a drug used to treat hypercalcemia (too much
calcium in the blood). Patients who stop taking tenofovir DF because of bone toxicity
continue to be followed on the regular study schedule. Those who stop the drug for toxicity
other than bone toxicity or for toxicity not related to tenofovir DF are followed every 4
weeks until their laboratory test results improve.
Tenofovir disoproxil fumarate (TDF) was approved for the treatment of HIV-infected adults in
October 2001. In November 2001, we began enrollment to our phase I/II study of tenofovir DF
in HIV-infected children (02-C-0006). That study has completed enrollment. The virologic and
immunologic responses seen on that study in a group of heavily treatment-experienced
children with multidrug resistant HIV were surprisingly good. The drug was well tolerated,
but significant decreases in bone mineral density were seen in a minority of patients.
With the current study we will enroll and systematically investigate HIV-infected children
for whom tenofovir DF is being used as part of salvage combination HIV therapy. The primary
objective of the study is to characterize the change in bone mineral density (BMD), as
measured by lumbar spine dual-energy x-ray absorptiometry (DEXA), during and following
treatment with tenofovir DF-containing antiretroviral therapy in HIV-infected children. The
study will enroll 3 cohorts of children: 1) HIV-infected children about to start a tenofovir
DF-containing antiretroviral regimen, 2) HIV-infected children already on tenofovir DF with
available baseline DEXA results, and 3) HIV-infected children already on tenofovir DF but
without baseline DEXA results who will come here for investigations of bone metabolism.
Studies of bone metabolism will include periodic measurements of serum and urine calcium and
phosphorus, PTH and vitamin D levels, bone resorption markers (urinary collagen cross-linked
N-telopeptide and free deoxypyridinoline), bone formation markers (serum osteocalcin and
bone specific alkaline phosphatase), IGF-1 levels, bone age, and DEXA scans. Patients about
to start tenofovir DF (cohort 1) will be offered the option of having a transiliac crest
core bone biopsy with tetracycline labeling performed at baseline and at 6 months to assess
static and dynamic parameters of bone quality and turnover (histomorphometry). Subjects with
substantial presumed tenofovir DF-related bone toxicity who are deriving benefit from their
tenofovir DF-containing antiretroviral drug regimen will be offered the option of
pamidronate therapy. The effects of pamidronate treatment on bone toxicity associated with
tenofovir DF in these patients will be assessed in an exploratory fashion. It is expected
that up to 40 patients with baseline BMD measurements will be enrolled onto this protocol.
An additional 10 patients who are undergoing tenofovir DF treatment but who did not receive
baseline BMD measurements will also be permitted to enroll in order to contribute to the
data used to characterize changes in toxicity.
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Endpoint Classification: Safety/Efficacy Study, Primary Purpose: Treatment
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