Ciafaloni Emma, Fox Deborah J, Pandya Shree, Westfield Christina P, Puzhankara Soman, Romitti Paul A, Mathews Katherine D, Miller Timothy M, Matthews Dennis J, Miller Lisa A, Cunniff Christopher, Druschel Charlotte M, Moxley Richard T
Department of Neurology, University of Rochester, Rochester, NY, USA.
J Pediatr. 2009 Sep;155(3):380-5. doi: 10.1016/j.jpeds.2009.02.007. Epub 2009 Apr 25.
To identify key factors for the delay in diagnosis of Duchenne muscular dystrophy (DMD) without known family history.
The cohort comes from the Muscular Dystrophy Surveillance, Tracking, and Research Network (MD STARnet), a multistate, multiple-source, population-based surveillance system that identifies and gathers information on all cases of Duchenne and Becker muscular dystrophy born since 1982. We analyzed medical records of 453 Duchenne and Becker muscular dystrophy boys to document the time course and steps taken to reach a definitive diagnosis.
Among 156 boys without known family history of DMD prior to birth, first signs or symptoms were noted at a mean age of 2.5 years. Concerns resulted in primary care provider evaluation of the child at a mean age of 3.6 years. Mean age at time of initial creatine kinase was 4.7 years. Mean age at definitive diagnosis of DMD was 4.9 years.
There is a delay of about 2.5 years between onset of DMD symptoms and the time of definitive diagnosis, unchanged over the previous 2 decades. This delay results in lost opportunities for timely genetic counseling and initiation of corticosteroid treatment. We recommend checking creatine kinase early in the evaluation of boys with unexplained developmental delay.
确定无已知家族病史的杜氏肌营养不良症(DMD)诊断延迟的关键因素。
该队列来自肌肉萎缩症监测、追踪和研究网络(MD STARnet),这是一个多州、多源、基于人群的监测系统,可识别并收集自1982年以来出生的所有杜氏和贝克肌营养不良症病例的信息。我们分析了453名杜氏和贝克肌营养不良症男孩的病历,以记录确诊过程的时间进程和所采取的步骤。
在出生前无DMD已知家族病史的156名男孩中,首次出现体征或症状的平均年龄为2.5岁。家长的担忧导致初级保健提供者在平均年龄3.6岁时对孩子进行评估。首次检测肌酸激酶时的平均年龄为4.7岁。DMD确诊时的平均年龄为4.9岁。
DMD症状出现与确诊时间之间存在约2.5年的延迟,在过去20年中没有变化。这种延迟导致错失及时进行遗传咨询和开始使用皮质类固醇治疗的机会。我们建议在评估不明原因发育迟缓的男孩时尽早检查肌酸激酶。
