Gross Motor Function in Pediatric Onset TUBB4A-Related Leukodystrophy: GMFM-88 Performance and Validation of GMFC-MLD in TUBB4A.

IF 2 4区 医学 Q3 CLINICAL NEUROLOGY Journal of Child Neurology Pub Date : 2023-08-01 Epub Date: 2023-07-17 DOI:10.1177/08830738231188159
Francesco Gavazzi, Virali Patel, Brittany Charsar, Allan Glanzman, Jacqueline Erler, Anjana Sevagamoorthy, Emma McKenzie, Tracy Kornafel, Elizabeth Ballance, Samuel R Pierce, Michelle Teng, Brielle Formanowski, Sarah Woidill, Justine Shults, Evangeline Wassmer, Davide Tonduti, Francesca Magrinelli, Geneviève Bernard, Marjo Van Der Knaap, Nicole Wolf, Laura Adang, Adeline Vanderver
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Abstract

TUBB4A pathogenic variants are associated with a spectrum of neurologic impairments including movement disorders and leukodystrophy. With the development of targeted therapies, there is an urgent unmet need for validated tools to measure mobility impairment. Our aim is to explore gross motor function in a pediatric-onset TUBB4A-related leukodystrophy cohort with existing gross motor outcome tools. Gross Motor Function Measure-88 (GMFM-88), Gross Motor Function Classification System (GMFCS-ER), and Gross Motor Function Classification-Metachromatic Leukodystrophy (GMFC-MLD) were selected through face validity. Subjects with a confirmed clinical and molecular diagnosis of TUBB4A-related leukodystrophy were enrolled. Participants' sex, age, genotype, and age at disease onset were collected, together with GMFM-88 and concurrent GMFCS-ER and GMFC-MLD. Performances on each measure were compared. GMFM-88 floor effect was defined as total score below 20%. A total of 35 subjects participated. Median performance by GMFM-88 was 16.24% (range 0-97.31), with 42.9% (n = 15) of individuals performing above the floor. GMFM-88 Dimension A (Lying and Rolling) was the best-performing dimension in the GMFM-88 (n = 29 above the floor). All levels of the Classification Scales were represented, with the exception of the GMFC-MLD level 0. Evaluation by GMFM-88 was strongly correlated with the Classification Scales (Spearman correlations: GMFCS-ER:GMFM-88 r = 0.90; GMFC-MLD:GMFM-88 r = 0.88; GMFCS-ER:GMFC-MLD: r = 0.92). Despite overall observation of a floor effect, the GMFM-88 is able to accurately capture the performance of individuals with attenuated phenotypes. GMFM-88 Dimension A shows no floor effect. GMFC-MLD shows a strong correlation with GMFCS-ER and GMFM-88, supporting its use as an age-independent functional score in TUBB4A-related leukodystrophy.

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儿童发病性TUBB4A相关白细胞营养不良的毛运动功能:GMFM-88在TUBB4A中的表现和GMFC-MLD的验证。
TUBB4A致病性变体与一系列神经损伤有关,包括运动障碍和白细胞营养不良。随着靶向疗法的发展,对测量行动障碍的有效工具的需求迫切未得到满足。我们的目的是利用现有的毛运动结果工具,在儿科发病的TUBB4A相关白质营养不良队列中探索毛运动功能。通过面孔有效性选择毛运动功能测量88(GMFM-88)、毛运动功能分类系统(GMFCS-ER)和毛运动功能分级中色性白质营养不良(GMFC-MLD)。入选了经临床和分子诊断为TUBB4A相关白细胞营养不良的受试者。收集参与者的性别、年龄、基因型和发病年龄,以及GMFM-88和同时发生的GMFCS-ER和GMFC-MLD。比较了每种测量方法的性能。GMFM-88地板效应定义为总分低于20%。共有35名受试者参加。GMFM-88的中位表现为16.24%(范围0-97.31),42.9%(n = 15) 在地板上表演的个人。在GMFM-88(n = 29)。除GMFC-MLD 0级外,所有级别的分类量表都有代表性。GMFM-88的评估与分类量表密切相关(Spearman相关性:GMFCS-ER:GMFM-88r = 0.90;GMFC-MLD:GMFM-88 r = 0.88;GMFCS-ER:GMFC-MLD:r = 0.92)。尽管总体上观察到了地板效应,但GMFM-88能够准确地捕捉表型减弱的个体的表现。GMFM-88尺寸A未显示地板效果。GMFC-MLD显示出与GMFCS-ER和GMFM-88的强相关性,支持其作为TUBB4A相关白质营养不良的年龄无关功能评分。
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来源期刊
Journal of Child Neurology
Journal of Child Neurology 医学-临床神经学
CiteScore
4.20
自引率
5.30%
发文量
111
审稿时长
3-6 weeks
期刊介绍: The Journal of Child Neurology (JCN) embraces peer-reviewed clinical and investigative studies from a wide-variety of neuroscience disciplines. Focusing on the needs of neurologic patients from birth to age 18 years, JCN covers topics ranging from assessment of new and changing therapies and procedures; diagnosis, evaluation, and management of neurologic, neuropsychiatric, and neurodevelopmental disorders; and pathophysiology of central nervous system diseases.
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