Epidemiology of scoliosis in cerebral palsy: A population‐based study at skeletal maturity

粗大运动功能分类系统 医学 脊柱侧凸 脑瘫 柯布角 队列 痉挛 人口 物理疗法 队列研究 儿科 外科 内科学 环境卫生
作者
Kate Willoughby,Soon Ang,Pam Thomason,Erich Rutz,Benjamin J. Shore,Aaron J. Buckland,Michael B. Johnson,Kerr Graham
出处
期刊:Journal of Paediatrics and Child Health [Wiley]
卷期号:58 (2): 295-301 被引量:8
标识
DOI:10.1111/jpc.15707
摘要

Aim This study investigated the prevalence of scoliosis in a large, population‐based cohort of individuals with cerebral palsy (CP) at skeletal maturity to identify associated risk factors that may inform scoliosis surveillance. Methods Young people with CP born between 1990 and 1992 were reviewed through routine orthopaedic review or a transition clinic. Classification of CP was recorded by movement disorder, distribution, gross and fine motor function. Clinical examination was undertaken and those with clinical evidence of scoliosis or risk factors had radiographs of the spine. Scoliosis severity was measured and categorised by Cobb angle. Results Two hundred and ninety‐two individuals were evaluated (78% of the birth cohort) at a mean age of 21 years, 4 months (range 16–29 years). Scoliosis (Cobb angle >10°) was found in 41%, with strong associations to the Gross Motor Function Classification System (GMFCS), Manual Abilities Classification System (MACS) and dystonic/mixed movement disorders. Those at GMFCS V were 23.4 times (95%CI 9.9–55.6) more likely to develop scoliosis than those at GMFCS I. Severe curves (Cobb >40°, 13% of the cohort) were found almost exclusively in those functioning at GMFCS IV and V, and were 18.2 times (95%CI 6.9–48.5) more likely to occur in those with dystonia than those with spasticity. Conclusions Scoliosis was very common in young people with CP, with prevalence and severity strongly associated with GMFCS and MACS level and dystonic movement disorder. Severe curves were almost exclusively found in non‐ambulant children. Clinical screening for scoliosis should occur for all children with CP, with radiographic surveillance focusing on those functioning at GMFCS IV and V.
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