Profiling Scoliosis in Rett Syndrome

被引:0
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作者
Alan K Percy
Hye-Seung Lee
Jeffrey L Neul
Jane B Lane
Steven A Skinner
Suzanne P Geerts
Fran Annese
Joy Graham
Lauren McNair
Kathleen J Motil
Judy O Barrish
Daniel G Glaze
机构
[1] University of Alabama at Birmingham,Department of Pediatrics
[2] University of South Florida,Department of Pediatrics
[3] Baylor College of Medicine,Department of Pediatrics
[4] Greenwood Genetic Center,undefined
来源
Pediatric Research | 2010年 / 67卷
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摘要
To understand scoliosis, related comorbidities, and phenotype-genotype correlations in individuals with Rett syndrome (RTT), the Rare Disease Clinical Research Network database for RTT was probed. Clinical evaluations included a detailed history and physical examination, comprehensive anthropometric measurements, and two quantitative measures of clinical status, Clinical Severity Scale (CSS) and motor-behavioral analysis (MBA). All data were exported to the Data Technology Coordinating Center (DTCC) at the University of South Florida. Scoliosis assessment was based on direct examination and curvature measurements by radiography (Cobb angle). Statistical analyses included univariate and multiple logistic regression models, adjusting for age at enrollment or mutation type. Scoliosis data were available from 554 classic RTT participants, mean age = 10 y (0–57 y). Scoliosis was noted in 292 (53%); mean age = 15 y with scoliosis and 6 y without. Using multiple regression analysis, MBA severity score, later acquisition, loss or absent walking, and constipation were associated with scoliosis. Two common methyl-CpG-binding protein 2 (MECP2) mutations, R294X and R306C, had reduced risk for scoliosis. These findings corroborated previous reports on scoliosis and extended understanding of comorbidities, clinical severity, and relative risk reduction for specific mutations. Clinical trial design should account for scoliosis and related factors judiciously.
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页码:435 / 439
页数:4
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