Chen Yuyi, Yang Dongling, Huang Xuelin, Feng Juntan, Zhao Qingqing, Huang Huixian, Liang Lushi, Zhang Xinxin, Ruan Yiyan
Department of Pediatric Neurology, Maternal and Child Health Hospital of Guangxi Zhuang Autonomous Region, Nanning, China.
Front Neurol. 2024 Jul 15;15:1391613. doi: 10.3389/fneur.2024.1391613. eCollection 2024.
Spinal muscular atrophy (SMA) is a genetic progressive neuromuscular disease. Nusinersen is the first disease modifying drug approved to treat patients with SMA. Our study aimed to evaluate the efficacy of nusinersen treatment on motor function in children with SMA.
A retrospective analysis was conducted on the data of 52 genetically confirmed SMA patients from November 2020 to September 2023. Motor function was assessed based on standardized scales from baseline to 14 months of follow-up.
Of patients in this study, the majority had SMA type 2 (40/52, 76.9%), 5 (9.6%) and 7 (13.5%) patients had SMA types 1 and 3, respectively. The median disease duration was 11 months (range 0-52), and the median age at initiation of treatment was 44.5 months (range 5-192). Motor function of all the patients with SMA improved from baseline to 14 months of follow-up. Mean increases of 4.6-point ( = 0.173), 4.7-point ( = 0.021) and 2.7-point ( = 0.013) were observed from baseline to 14 months of follow-up for the Children's Hospital of Philadelphia Infant Test of Neuromuscular Disorders scores, the Hammersmith Functional Motor Scale Expanded (HFMSE) and the Revised Upper Limb Module (RULM), respectively. Increased disease duration and age of treatment initiation were negatively correlated with the changes in HFMSE scores ( = -0.567, = 0.043; = -0.771 and = 0.002, respectively). Similar results were observed for the RULM scores ( = -0.714, = 0.014; = -0.638 and = 0.035, respectively).
Our study suggested that 14 months of treatment with nusinersen was effective and improved the motor function of children with SMA types 1, 2, or 3. In addition, disease duration and age at treatment initiation were negatively correlated with treatment outcome in the patients.
脊髓性肌萎缩症(SMA)是一种遗传性进行性神经肌肉疾病。诺西那生钠是首个被批准用于治疗SMA患者的疾病修正药物。我们的研究旨在评估诺西那生钠治疗对SMA儿童运动功能的疗效。
对2020年11月至2023年9月期间52例基因确诊的SMA患者的数据进行回顾性分析。从基线到随访14个月,根据标准化量表评估运动功能。
本研究中的患者,大多数为2型SMA(40/52,76.9%),5例(9.6%)和7例(13.5%)患者分别为1型和3型SMA。疾病持续时间中位数为11个月(范围0 - 52),开始治疗时的年龄中位数为44.5个月(范围5 - 192)。所有SMA患者的运动功能从基线到随访14个月均有改善。从基线到随访14个月,费城儿童医院神经肌肉疾病婴儿测试评分、哈默史密斯功能运动量表扩展版(HFMSE)和修订上肢模块(RULM)的平均增加分别为4.6分(=0.173)、4.7分(=0.021)和2.7分(=0.013)。疾病持续时间增加和开始治疗的年龄与HFMSE评分变化呈负相关(分别为=-0.567,=0.043;=-0.771,=0.002)。RULM评分也观察到类似结果(分别为=-0.714,=0.014;=-0.638,=0.035)。
我们的研究表明,诺西那生钠治疗14个月是有效的,改善了1型、2型或3型SMA儿童的运动功能。此外,疾病持续时间和开始治疗的年龄与患者的治疗结果呈负相关。
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