Growth Hormone and Chromosome 18q- and Abnormal Growth
Information source: The University of Texas Health Science Center at San Antonio
ClinicalTrials.gov processed this data on August 23, 2015 Link to the current ClinicalTrials.gov record.
Condition(s) targeted: Chromosome 18; Growth Hormone Deficiency
Intervention: Nutropin AQ (Drug); Arginine and Clonidine Stimulation Testing (Procedure); Growth Factors Laboratory Testing (Procedure); Neuropsychological Testing (Procedure)
Phase: Phase 3
Status: Active, not recruiting
Sponsored by: The University of Texas Health Science Center at San Antonio Official(s) and/or principal investigator(s): Daniel E. Hale, M.D., Principal Investigator, Affiliation: The University of Texas Health Science Center at San Antonio
Summary
We, the investigators at the University of Texas Health Science Center at San Antonio, want
to learn if height and IQ (intelligence quotient) scores are improved by growth hormone (GH)
treatment in children with chromosome 18 deletions and abnormal growth. Data from a
previous study showed that growth hormone improved height in all children with 18q- and
growth hormone deficiency. In addition, most of the study participants on growth hormone
treatment showed an increase in IQ scores.
Clinical Details
Official title: Growth Hormone Trial for Children With 18q- and Abnormal Growth
Study design: Allocation: Non-Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Diagnostic
Primary outcome: growth rates 12-15 months after treatment begins
Secondary outcome: performance IQ scores 12-15 months after treatment begins
Detailed description:
HYPOTHESIS:
Our hypothesis with reference to children with 18q deletions who have abnormal growth are:
- growth hormone will improve growth; and
- growth hormone will improve performance IQ (pIQ).
Therefore, our specific aims are to evaluate the impact of GH treatment on:
- linear growth in children with 18q deletions who have abnormal growth but who are not
classically growth hormone deficient; and
- pIQ in children with 18q deletions who have abnormal growth
GOALS AND METHODS:
We have already investigated the growth axis in 50 individuals with a cytogenetically and
molecularly confirmed 18q deletion by determining the height, growth velocity, insulin-like
growth factor 1 (IGF1), IGF binding protein 3 (IGFBP3), bone maturation and growth hormone
(GH) response to pituitary stimulants (clonidine and arginine). To summarize: children
with 18q deletions are short: 64% have a height more than 2 S. D. below the mean. Affected
children also grow slowly: 68% have a growth velocity more than 1 S. D. below the mean.
Half of the individuals have delayed bone maturation. Growth factors are skewed downward:
72% of the IGF1 values and 83% of the IGFBP3 values are below the average for normal
children. Similarly, 72% of the children failed to adequately respond to the GH stimulants.
In the total group of 50 children, 20 (40%) were classically GH DEFICIENT (height <-2 S. D.,
velocity <-1 S. D., bone age <-2 S. D., IGF1 < - 1 S. D., IGFBP3 <-1 S. D., peak GH <10 ng/ml by
polyclonal GH assay) and are on GH treatment. Of the remaining 30 children, 28 have
multiple abnormalities of the growth axis, primarily growth velocity <-1 S. D. (ABNORMAL
GROWTH), but did not qualify for GH treatment according to criteria set by their private
insurer. Almost all of these children had abnormalities suggestive of hypothalamic
dysfunction involving TSH and prolactin. None have CNS abnormalities of the pituitary on
MRI. Thus we suspect that many of these children hve neurosecretory dysfunction. Parental
heights are slightly above average (father HTZ = 0. 3 +/- 1. 2, mother HTZ = 0. 1 +/- 1. 1) and
none of the children are overweight.
Of 8 children with GHD on prolonged GH treatment, growth rates are comparable to those
reported by the NCGS for idiopathic GHD at 1 and 2 years. The mean change in height over a
28-month period for the treated group in our study was +1. 8 S. D. while it was - 0. 25 S. D. in
the untreated group (p<0. 001). No known complications of GH treatment were encountered.
Furthermore, because of an association between 18q deletion, hypomyelination and cognition,
some non-statural benefits of GH treatment were examined: specifically, the performance
intelligence quotient (pIQ) was measured using a detailed battery of neuropsychological
instruments. The pIQ was measured because many of the children are hearing impaired and a
full scale IQ, which relies on verbal skills, would underestimate their abilities. The
GH-treated group was compared to an untreated group. The GH-treated group (n=8) showed an
increase in pIQ of 23 points (range 0 to +47) while the untreated group (n=6) showed no
change (range - 2 to +6)(p=0. 003). Based on these observations, we conclude that GHD
children with 18q deletions respond favorably to GH therapy in terms of both linear growth
and pIQ. In contrast, children with 18q deletions with abnormal growth who are not
classically GH deficient, show little change in height S. D. and pIQ over time. Therefore,
we propose to study (NEW STUDY) whether children with 18q deletions with abnormal growth can
benefit from GH treatment. For purposes of this proposal, abnormal growth is defined as a
growth velocity <-1 S. D.
Initial auxology, endocrine testing, and neurocognitive evaluation will be performed at our
Center. Auxologic and neurocognitive testing will be repeated after 18 months of therapy at
our Center. These studies are done at our Center to assure consistency of evaluation, which
is a particular concern for the neurocognitive tests. Many of the children will also
participate in other studies in our Center (MRI imaging, psychological evaluations of family
function) that are not part of this application. Children begun on GH treatment will need
to be seen by a pediatric endocrinologist for dosage adjustment after 3, 6, 9 and 12 months.
The untreated children will also need to be seen by a pediatric endocrinologist for
auxologic studies at the same time points. We enrolled 20 children in this study. Few of
the children are located in any single geographic area; therefore, we will have 12-20
centers seeing individual children. Rather than developing new forms, standard NCGS intake
forms will be used for the intermediate visits by the local pediatric endocrinologists.
Control Group: We have more than 20 previously studied children, 5. 3 +/- 2. 8 years of age,
who have abnormal growth and have never received GH. All have undergone extensive
auxologic, hormonal, neurocognitive and neuroimaging evaluations. These studies were done
15. 4 +/- 9 months ago (range 11-28 months). We have already shown that, in the absence of
intervention, height S. D. and pIQ are stable over time; therefore, these children can serve
as their own controls.
We also have 20 children who are GH deficient and on treatment that are participants in
another study. These children were evaluated prior to the initiation of treatment. All are
scheduled to be re-evaluated at least twice in a five-year period. The data on the first 8
treated children were reported above. These children will serve as important "disease
controls".
NAME OF FDA APPROVED DRUG TO BE USED:
We are using Nutropin AQ in this study.
METHOD OF TREATMENT ASSIGNMENT:
All children who have previously been evaluated in our Center were offered the opportunity
to receive GH, subject to the following limitations:
- The prior evaluation must have occured at least 12 months preceding the anticipated
date of initiation of GH therapy.
- May not be on GH treatment or have been previously treated with GH
- Growth velocity <-1 S. D. with normal weight for length/height
- Be willing to return to our Center for reevaluation of auxologic parameters and
neurocognitive testing prior to the initiation of GH therapy.
- Be willing to administer GH on a daily basis for 12-15 months
- Be willing to return to our Center for re-evaluation after 12-15 months of therapy.
The majority of the 20 patients for this study came from the group of children who have been
previously evaluated.
New children (families) being seen for their initial visit in our Center, will be offered
the opportunity to participate in the clinical trial if they have abnormal growth and are
not classically GHD. However, these children will be randomly assigned either to treatment
or non-treatment for the initial 12-month period. Both treated and untreated children
(families) must comply with limitations 2-6 above.
The minority of the 20 patients for this study came from the group of children who are new.
TYPE OF RANDOMIZATION:
Randomization applied only to children who are new to our Center. When the results of
growth factor and GH provocative testing are known, a two-step process will occur.
Children, who are GHD, will be started on GH and entered into an on-going study already
underway in our Center. They will not qualify for participation in the proposed NEW study.
Children who have abnormal growth will be assigned to either the treatment or non-treatment
category, using an adaptive randomization scheme to avoid imbalances in the numbers of
subjects allocated to the two groups.
PLANNED INTERIM ANALYSIS:
GH-treated children will be seen at 3, 6, 9 and 12 months by their local pediatric
endocrinologist for measurement of height and weight, review of medical history and dosage
adjustment. Untreated children will be seen at 3, 6, 9, and 12 months for measurement of
height and weight and review of medical history.
Eligibility
Minimum age: N/A.
Maximum age: 18 Years.
Gender(s): Both.
Criteria:
Inclusion Criteria:
- Diagnosis of chromosome 18 deletion (cytogenetics report)
- Children with abnormal growth but who are not classically growth hormone deficient
Exclusion Criteria:
- Children previously on growth hormone therapy
Locations and Contacts
The University of Texas Health Science Center at San Antonio, San Antonio, Texas 78229-3900, United States
Additional Information
Starting date: February 2001
Last updated: July 17, 2007
|