Karin Forsberg, Merete Karlsborg, Lisette Salvesen, Kirsten Svenstrup, Ivar Winroth, Henrik Berntsson, Peter M Andersen
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引用次数: 0
摘要
我们介绍了一名因 SOD1 基因中的侵袭性 A4S 突变而导致的家族性肌萎缩侧索硬化症患者。2020 年,该患者被纳入 VALOR SOD1 基因疗法第三阶段试验。筛查时,ALSFRS-R 评分为 41 分(48 分为正常),CSF-神经丝 L 水平(持续神经元损伤的指标)为 11 000 纳克/升(参考文献)。
[SOD1 gene therapy delays ALS disease progression].
We present a patient with familial amyotrophic lateral sclerosis caused by an aggressive A4S mutation in the SOD1 gene. In 2020, the patient was enrolled in the VALOR SOD1 gene therapy phase-3 trial. At screening, the ALSFRS-R score was 41 (48 is normal) and the level of CSF-neurofilament L (an indicator of ongoing neuronal damage) was 11 000 ng/L (ref <650 ng/L). In the four years following enrollment, the patient received monthly intrathecal treatment with tofersen, an antisense oligonucleotide compound that inhibits SOD1 protein expression and hence lowers the synthesis of toxic SOD1 protein species. Side effects have been minimal and mostly attributed to the spinal taps. The patient remains ambulatory with an active social lifestyle. The ALSFRS-R score has in the past 18 months stabilized around 35-37, CSF-NfL is 1 290 ng/L and plasma-NfL is 12 (reference <13). This is the first documented arresting intervention in a patient with ALS in Sweden.
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