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KMID : 1036920160210010015
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Annals of Pediatric Endocrinology & Metabolism
2016 Volume.21 No. 1 p.15 ~ p.20
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Endocrine dysfunctions in children with Williams-Beuren syndrome
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Kim Yoon-Myung
Cho Ja-Hyang
Kang Eun-Gu
Kim Gu-Hwan
Seo Eul-Ju
Lee Beom-Hee
Choi Jin-Ho
Yoo Han-Wook
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Abstract
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Purpose: Williams-Beuren syndrome (WBS) is caused by a hemizygous microdeletion of chromosome 7q11.23 and is characterized by global cognitive impairment, dysmorphic facial features, and supravalvular aortic stenosis. Endocrine dysfunctions have been reported in patients with WBS. This study was performed to investigate the frequency, clinical features, and outcomes of endocrine dysfunctions in children with WBS.
Methods: One hundred two patients were included. The diagnosis was confirmed by chromosome analysis and fluorescent in situ hybridization. Medical charts were reviewed retrospectively to analyze endocrine dysfunctions such as short stature, precocious puberty, thyroid dysfunctions, and hypocalcemia.
Results: The age at diagnosis was 3.7¡¾4.4 years (one month to 19 years). Height- and weight-standard deviation score (SDS) were ?1.1¡¾1.1 and ?1.4¡¾1.4 at presentation, respectively. Short stature was found in 26 patients (28.3%) among those older than 2 years. Body mass index-SDS increased as the patients grew older (P<0.001). Two males and one female (2.9%) were diagnosed with central precocious puberty. Nine patients (8.8%) were diagnosed with primary hypothyroidism at age 4.0¡¾4.3 years (one month to 12.1 years); their serum thyroid stimulating hormone and free T4 levels were 15.2¡¾5.4 ¥ìU/mL and 1.2¡¾0.2 ng/dL, respectively. Hypercalcemia was observed in 12 out of 55 patients under age 3 (22%) at the age of 14.3¡¾6.6 months (7 to 28 months) with a mean serum calcium level of 13.1¡¾2.1 mg/dL.
Conclusion: Endocrine dysfunctions are not uncommon causes of morbidity in patients with WBS. The severity and outcomes of their endocrine manifestations were heterogeneous. Long-term follow-up is needed to predict the prognosis of endocrine features.
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KEYWORD
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Hypercalcemia, Precocious puberty, Short stature, Hypothyroidism, Williams-Beuren syndrome
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