Williams syndrome (WS) is a rare microdeletion genetic disorder that has a broad phenotype including many endocrine and metabolic abnormalities. Dr. Pober and colleagues at MGH have reported the following findings in adults with WS: abnormal body composition (excess body fat accumulation with a lipedema phenotype), decreased bone mineral density, abnormal glucose tolerance, and reduced lean mass. Despite the high prevalence and potential effect of metabolic abnormalities on the health of persons with WS, their full phenotypic range, potential causal factors (either genetic and/or hormonal) along with their impact on other aspects of health (such as risk of falls and fractures or interaction with emotional behavioral concerns) remain incompletely characterized. The purpose of the current study in a large cohort of subjects with WS is to: collect further information to characterize the timing of onset and distribution of body fat; better characterize hormonal status of WS subjects; and screen for genetic variation using single-nucleotide-polymorphism (SNP) analysis that could elucidate genetic contributors to the lipedema phenotype as well as the other observed metabolic and bone abnormalities.
Study Type
OBSERVATIONAL
Enrollment
144
Massachusetts General Hospital
Boston, Massachusetts, United States
Bone Mineral Density - Lumbar Spine
Time frame: baseline only
Whole Body DEXA (dual energy x-ray absorptiometry) scan
To assess body proportions of fat, bone, and muscle
Time frame: baseline only
Bone Mineral Density - Hip
Time frame: baseline only
Resting energy expenditure
Time frame: baseline only
Serum Total Testosterone
Time frame: baseline only
Serum Estrogen
Time frame: baseline only
Fasting blood sugar and Oral glucose tolerance test (OGTT)
Time frame: baseline only
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