The aim of this study is to study the effects of GH on body composition, lipid and glucose metabolism, physical performance and safety aspects in adults with PWS.The patients are randomized to either GH or placebo the first year of the study, subsequently followed by two years of GH treatment. the study is performed in Norway, Sweden and Denmark.
OBJECTIVE(S): Prader Willi syndrome (PWS) is a multi-symptomatic genetic disorder associated with abnormalities in the growth hormone (GH)-insulin-like-growth factor (IGF)-I axis and in the body composition. GH treatment is a registered indication in children with PWS, and improves growth rate and body composition. One pilot study in adult patients with clinical PWS has shown beneficial effects on body composition without simultaneous significant side effects. The aim of the present study is to evaluate the effects of GH treatment on body composition, muscle function and quality of life in PWS adults. TRIAL DESIGN: The study will be an investigator initiated and investigator sponsored multinational and multi-centre trial, including centres in Norway, Sweden and Denmark. Within each centre patients will be randomised (double blind) to one year treatment with daily injections of GH or placebo (efficacy), followed by a two year observation period on GH treatment (safety). TRIAL POPULATION: Twenty patients from each centre are included in the study. The patients need a genetically verified diagnosis and should be between 18 and 40 years old. Patients are excluded if GH treatment has been given within the last two years, if they have a malignancy or other serious diseases, in particular severe respiratory diseases. ASSESSMENTS: Effect is evaluated primarily as changes in body composition, activity of daily living and quality of life. SAFETY: Before starting in the study all patients will be examined for tonsillary hypertrophy and sleep apnoea. Oral Glucose Tolerance Tests will be performed regularly. TRIAL PRODUCT(S): During the initial 4 weeks of the placebo-controlled study phase patients will be treated with sc injections of GH (Norditropin Simplexx) in the evening with doses of 0.3 mg/day respectively 0.4 mg/day if BW is below or above 100 kg. Thereafter doses will be increased to 0.6 mg/day (0.8 mg/day) and maintained fixed for 11 months. During the following 24 months open phase doses will be individually titrated.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
TRIPLE
Enrollment
46
0.3-0.4 mg/day placebo or GH for 4 weeks. Thereafter 0.6-0.8 mg/day placebo or GH for 11 months. During the following 24 months open phase doses will be individually titrated.
Center for rare Diseases, Department of Pediatrics, Skejby University Hospital
Aarhus N, Denmark
Endokrinologisk seksjon, Med Avd, Rikshospitalet
Oslo, Norway
Department of Endocrinology and Diabetology, Karolinska Hospital
Stockholm, Sweden
Changes in body composition (lean body mass and fat mass) measured by dual energy X-ray absorptiometry (DXA)
Time frame: 36 months
Bone mineral density measured by DXA
Time frame: 36 months
Effects on forced expiratory volume (Peakflow)
Time frame: 36 months
Standard photography appearance according to visual analogue scale (VAS)
Time frame: 36 months
Effects on free and total IGF-I, IGF-binding protein (BP)-1 and 3
Time frame: 36 months
Effects on lipids (fasting triglycerides(TG), total, HDL and LDL cholesterol)
Time frame: 36 months
Effects on body composition measured with bioimpedance
Time frame: 36 months
Effects on haemoglobin (Hb), leucocyte and thrombocyte counts, FSH, LH, estradiol, Testosterone, inhibin B, TSH and Thyroxine
Time frame: 36 months
Muscle and fat mass measured by abdominal and mid-femoral computerized tomography
Time frame: 36 months
Activity of daily living measured a.m. Guralnik
Time frame: 36 months
Quality of life estimated by questionnaires
Time frame: 36 months
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