The real-world impact of biologics for NMOSD: A retrospective single-center study compared with natural course and conventional treatments in Japanese

IF 2.9 3区 医学 Q2 CLINICAL NEUROLOGY Multiple sclerosis and related disorders Pub Date : 2024-11-16 DOI:10.1016/j.msard.2024.106176
Naoya Yamazaki , Tatsuro Misu , Yuki Matsumoto , Yoshiki Takai , Chihiro Namatame , Hirohiko Ono , Kimihiko Kaneko , Shuhei Nishiyama , Hiroshi Kuroda , Toshiyuki Takahashi , Ichiro Nakashima , Kazuo Fujihara , Masashi Aoki
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Abstract

Background

Neuromyelitis optica spectrum disorder (NMOSD), a central nervous system inflammatory disease associated with aquaporin-4 immunoglobulin G (AQP4-IgG), is conventionally treated with oral steroids and immunosuppressants (IS) in Japan. Several biologics which show great efficacy in the clinical trials have been developed recently. However, studies on their efficacy, especially those comparing them with conventional treatments in real-world situations are lacking.

Objective

Here, we conducted a single-center retrospective cohort study in Japan comparing the efficacy of biologics, over conventional drugs, in treating AQP4-IgG-positive NMOSD.

Methods

We extracted the medical history of patients with AQP4-IgG-positive NMOSD who visited the Tohoku University Hospital between 2000 and 2023, from the hospital patient database. All patients were diagnosed according to the international consensus diagnostic criteria for NMOSD 2015. We then classified the disease duration of each patient into four periods based on their prescription history as: no-treatment, prednisolone monotherapy (PSL-mono), immunosuppressants (IS) treatment, and biologics (Bio) treatment. Subsequently, the efficacy of Bio treatment, over the conventional treatment, in alleviating AQP4-IgG-positive NMOSD was estimated. We used univariate Poisson regression analysis to compare the annualized relapse rate (ARR), log-rank test for the first attack, and the hazard ratios (HR)—calculated using multivariate Andersen-Gill model for recurrent attacks—of the Bio and conventional treatment period groups. The safety of each treatment period group was assessed by comparing infection and mortality rates.

Results

A total of 109 patients (92 % females) met the eligibility criteria of the study. We could extract a total of 1,283 patient years with 289 NMOSD attacks from their medical history data. The mean ARR of no-treatment group was 0.60. Most of the Bio group initially received combined treatments with PSL or IS. The mean ARR of the Bio group was 0.01 [95 % confidence interval (CI): 0.002 to 0.08], which was significantly lower than the PSL-mono group (0.16, 95 % CI: 0.13 to 0.19, p = 0.03) and the IS group (0.17, 95 % CI: 0.13 to 0.22, p = 0.02). In the survival analysis, the Bio group showed a significantly prolonged attack-free period than the other groups, suggesting its potential in reducing 79 % of relapses in the no-treatment group, 33 % in the PSL-mono group, and 31 % in the IS group during the two years. The multivariate analysis using Andersen-Gill model showed that the Bio group had significantly lower HR (log HR −2.75, 95 % CI: −4.71 to −0.8, p = 0.006), relative to the PSL-mono group. Importantly, the patients needed significantly lower PSL (median 5 mg/day) during the Bio group treatment period than in the PSL-mono group treatment period (median 10 mg/day). Further, the concomitant use of IS could be stopped safely in all patients who were on Bio treatment. All treatment period groups showed similar safety profiles.

Conclusion

In patients with AQP4-IgG-positive NMOSD, biologics demonstrated more efficacy than conventional PSL and/or IS treatment, without increasing infection and mortality rates.
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生物制剂对 NMOSD 的实际影响:在日本进行的一项回顾性单中心研究,与自然病程和传统疗法进行比较。
背景:神经脊髓炎视网膜频谱紊乱症(NMOSD)是一种与水通道蛋白-4 免疫球蛋白 G(AQP4-IgG)相关的中枢神经系统炎症性疾病,在日本通常采用口服类固醇和免疫抑制剂(IS)治疗。最近开发出了几种在临床试验中显示出巨大疗效的生物制剂。目的:在此,我们在日本开展了一项单中心回顾性队列研究,比较生物制剂与传统药物在治疗 AQP4-IgG 阳性 NMOSD 方面的疗效:我们从医院的患者数据库中提取了2000年至2023年间在东北大学医院就诊的AQP4-IgG阳性NMOSD患者的病史。所有患者均根据 2015 年 NMOSD 国际共识诊断标准进行诊断。然后,我们根据处方史将每位患者的病程分为四个时期:无治疗、泼尼松龙单药治疗(PSL-mono)、免疫抑制剂(IS)治疗和生物制剂(Bio)治疗。随后,我们估算了生物制剂治疗对缓解 AQP4-IgG 阳性 NMOSD 的疗效。我们使用单变量泊松回归分析比较了生物治疗组和常规治疗组的年复发率(ARR)、首次发作的对数秩检验以及复发的危险比(HR)(使用多变量安徒生-吉尔模型计算)。通过比较感染率和死亡率,评估了各治疗期组的安全性:共有 109 名患者(92% 为女性)符合研究资格标准。我们从他们的病史资料中提取了共 1,283 个患者年,其中有 289 次 NMOSD 发作。无治疗组的平均 ARR 为 0.60。大多数生物组患者最初接受了 PSL 或 IS 的联合治疗。生化组的平均急性发作率为 0.01 [95 % 置信区间 (CI):0.002 至 0.08],明显低于 PSL 单药组(0.16,95 % CI:0.13 至 0.19,P = 0.03)和 IS 组(0.17,95 % CI:0.13 至 0.22,P = 0.02)。在生存期分析中,Bio 组的无发作期明显比其他组长,这表明该疗法有可能在两年内减少 79% 的复发率(未治疗组)、33% 的复发率(PSL-mono 组)和 31% 的复发率(IS 组)。使用 Andersen-Gill 模型进行的多变量分析表明,与 PSL 单药组相比,Bio 组的 HR 显著降低(对数 HR -2.75,95 % CI:-4.71 至 -0.8,p = 0.006)。重要的是,患者在 Bio 组治疗期间所需的 PSL(中位数为 5 毫克/天)明显低于 PSL-mono 组治疗期间所需的 PSL(中位数为 10 毫克/天)。此外,所有接受 Bio 治疗的患者均可安全停用 IS。所有治疗组都显示出相似的安全性:对于AQP4-IgG阳性的NMOSD患者,生物制剂比传统的PSL和/或IS治疗更有效,同时不会增加感染率和死亡率。
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来源期刊
CiteScore
5.80
自引率
20.00%
发文量
814
审稿时长
66 days
期刊介绍: Multiple Sclerosis is an area of ever expanding research and escalating publications. Multiple Sclerosis and Related Disorders is a wide ranging international journal supported by key researchers from all neuroscience domains that focus on MS and associated disease of the central nervous system. The primary aim of this new journal is the rapid publication of high quality original research in the field. Important secondary aims will be timely updates and editorials on important scientific and clinical care advances, controversies in the field, and invited opinion articles from current thought leaders on topical issues. One section of the journal will focus on teaching, written to enhance the practice of community and academic neurologists involved in the care of MS patients. Summaries of key articles written for a lay audience will be provided as an on-line resource. A team of four chief editors is supported by leading section editors who will commission and appraise original and review articles concerning: clinical neurology, neuroimaging, neuropathology, neuroepidemiology, therapeutics, genetics / transcriptomics, experimental models, neuroimmunology, biomarkers, neuropsychology, neurorehabilitation, measurement scales, teaching, neuroethics and lay communication.
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