日本对依夫加替莫德治疗全身性肌萎缩症的疗效反应

IF 2.3 Q3 CLINICAL NEUROLOGY

Neurology. Clinical practice Pub Date : 2024-06-01 Epub Date: 2024-03-25 DOI:10.1212/CPJ.0000000000200276

Shigeaki Suzuki, Akiyuki Uzawa, Yuriko Nagane, Masayuki Masuda, Shingo Konno, Tomoya Kubota, Makoto Samukawa, Kei Ishizuchi, Daiki Tokuyasu, Hideo Handa, Manato Yasuda, Naoki Kawaguchi, Takashi Kimura, Yasushi Suzuki, Takamichi Sugimoto, Naoya Minami, Masanori P Takahashi, Hiroyuki Murai, Kimiaki Utsugisawa

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引用次数: 0

摘要

背景和目的：依加替莫德在全身性肌无力（MG）患者中具有良好的耐受性和疗效，在日本不仅可用于治疗抗乙酰胆碱受体阳性（AChR+）的全身性肌无力，还可用于治疗抗肌肉特异性受体酪氨酸激酶（MuSK+）和血清阴性的全身性肌无力。我们报告了在日本临床实践中使用依加替莫德治疗全身型 MG 的详细情况：我们纳入了日本肌无力注册（JAMG-R）研究小组2021年调查中的全身型肌无力患者，他们在2022年5月至9月期间接受了依加替莫德的初始周期治疗。我们将 "应答者 "定义为在首个治疗周期中MG日常生活活动（MG-ADL）得分≥2分的患者。我们还对 MG 综合评分和 15 项肌无力生活质量量表（MG-QOL15-r）修订版进行了评估：在1343名JAMG-R患者中，36人（2.7%）开始服用依加替莫德（女性占68%，年龄53岁）。他们的血清学特征如下AChR+, n = 19 (53%)；MuSK+, n = 6 (17%)；血清阴性，n = 11 (31%)。26名患者（72%）为难治性MG。在为期26周的观察期间，34名患者共接受了81个周期的依加替莫德治疗（平均2.4个周期）。两个周期之间的平均间隔为 5.9 周。在81个周期中，有65个周期（80%）每4周连续输注一次依加替莫德。在第一个周期，34 名患者的 MG-ADL 评分从 10.5 ± 4.3 显著降至 6.9 ± 5.1（p = 0.003）。同样，MG 综合评分和 MG-QOL15-r 评分的平均值也分别从 18.4 ± 13.6 降至 11.8 ± 9.6（p = 0.004）和从 19.2 ± 6.3 降至 14.2 ± 8.3（p = 0.007）。21名患者（62%）出现了应答。在随后的治疗周期中也观察到了治疗反应。有应答者服用依加替莫德的有效时间长短不一；4 名应答者只服用了一个有效周期。MuSK+患者的病情明显好转。7 名患者的泼尼松龙剂量有所减少。我们对患者干预后的状况进行了检查，发现有 6 名患者的症状表现极轻。5 名患者出现了 COVID-19。我们未能发现与应答者相关的临床或实验室结果：讨论：可以考虑将依加替莫德用于治疗表现不明显的全身型MG患者，在患者选择和治疗计划方面具有广泛的灵活性。

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Therapeutic Responses to Efgartigimod for Generalized Myasthenia Gravis in Japan.

Background and objectives: Efgartigimod, which has been well tolerated and efficacious in individuals with generalized myasthenia gravis (MG), is available in Japan not only for the treatment of anti-acetylcholine receptor-positive (AChR+) but also anti-muscle-specific receptor tyrosine kinase (MuSK+) and seronegative generalized MG. We report details of the use of efgartigimod for generalized MG in clinical practice in Japan.

Methods: We included patients with generalized MG in the 2021 survey of Japan Myasthenia Gravis Registry (JAMG-R) study group who received an initial cycle of efgartigimod between May and September 2022. We defined "responders" as patients who achieved a score ≥2 points for MG activities of daily living (MG-ADL) in the first treatment cycle. The MG composite and the Revised scale of the 15-item Myasthenia Gravis-Quality of Life scale (MG-QOL15-r) were also evaluated.

Results: Of 1,343 JAMG-R patients, 36 (2.7%) started efgartigimod (female 68%, age 53 years). Their serologic profiles were as follows: AChR+, n = 19 (53%); MuSK+, n = 6 (17%); and seronegative, n = 11 (31%). Twenty-six patients (72%) had refractory MG. There were 81 cycles of efgartigimod during the 26-week observation in 34 patients (average, 2.4 cycles). The mean interval between cycles was 5.9 weeks. A continuous 4-weekly infusion of efgartigimod was performed in 65 (80%) of 81 cycles. In the first cycle, the MG-ADL score of the 34 patients decreased significantly from 10.5 ± 4.3 to 6.9 ± 5.1 (p = 0.003). Similarly, the mean MG composite and MG-QOL15-r decreased from 18.4 ± 13.6 to 11.8 ± 9.6 (p = 0.004) and from 19.2 ± 6.3 to 14.2 ± 8.3 (p = 0.007), respectively. Twenty-one (62%) patients were responders. Therapeutic responses were observed in the subsequent cycles. The duration of effectiveness of efgartigimod was varied among the responders; 4 responders had only a single effective cycle. Significant improvement was observed in the MuSK+ patients. Prednisolone dose of 7 patients was reduced. Our examination of the patients' postintervention status revealed that 6 patients achieved minimal manifestations. COVID-19 occurred in 5 patients. We failed to detect clinical or laboratory findings associated with responders.

Discussion: Efgartigimod can be considered for the treatment of patients with generalized MG who do not achieve minimal manifestations, with a broad flexibility of patient selection and treatment schedules.

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来源期刊

Neurology. Clinical practice CLINICAL NEUROLOGY-

CiteScore

4.00

自引率

0.00%

发文量

期刊介绍： Neurology® Genetics is an online open access journal publishing peer-reviewed reports in the field of neurogenetics. The journal publishes original articles in all areas of neurogenetics including rare and common genetic variations, genotype-phenotype correlations, outlier phenotypes as a result of mutations in known disease genes, and genetic variations with a putative link to diseases. Articles include studies reporting on genetic disease risk, pharmacogenomics, and results of gene-based clinical trials (viral, ASO, etc.). Genetically engineered model systems are not a primary focus of Neurology® Genetics, but studies using model systems for treatment trials, including well-powered studies reporting negative results, are welcome.