重症肌无力生物靶向疗法的起始反应、最大疗效和治疗后效果：系统综述和网络荟萃分析。

IF 2.7 3区医学 Q2 CLINICAL NEUROLOGY

Frontiers in Neurology Pub Date : 2024-10-28 eCollection Date: 2024-01-01 DOI:10.3389/fneur.2024.1479685

Huahua Zhong, Zhijun Li, Xicheng Li, Zongtai Wu, Chong Yan, Sushan Luo, Chongbo Zhao

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引用次数: 0

摘要

背景：随着重症肌无力（MG）靶向药物开发的不断推进，比较这些药物的疗效以便更好地做出临床决策非常重要。然而，由于不同药物在临床试验中使用的治疗方案和剂量各不相同，因此有必要对它们进行标准化比较：本研究招募了参与治疗 MG 的创新靶向药物 II 期和 III 期试验的参与者。主要结果是肌无力定量评分（MG-QMG）与基线相比的变化。在四个时间点分别分析了所有药物的疗效：起始 1 周、起始 4 周、反应最大化和最后一次给药后 4 周。为了比较不同药物的疗效，研究人员进行了网络荟萃分析：共分析了12项研究中的9种药物，包括依加替莫德、罗扎尼珠单抗、巴妥珠单抗、依库珠单抗、贝利木单抗、齐鲁珠单抗、拉武珠单抗、尼泊珠单抗、利妥昔单抗。在起始的 1 周时间点，与安慰剂效果相比，有三种药物显示出显著的改善效果：这三种药物是：埃夫加替莫德（Efgartigimod）、齐鲁克普兰（Zilucoplan）和罗扎尼珠单抗（Rozanolixizumab）。在开始治疗的 4 周时间点，与安慰剂效果相比，有四种药物的疗效显著提高：依加替莫德、罗扎尼珠单抗、巴妥珠单抗和齐鲁珠单抗。在最大反应时间点，与安慰剂效果相比，有六种药物取得了明显改善：依加替莫德、罗扎诺利珠单抗、巴托珠单抗、Eculizumab、Zilucoplan、Ravulizumab。在最后一次给药后4周，所有药物在统计学上与安慰剂无显著差异：结论：尽管各项试验中的 MG 亚型并不一致，但在每项试验的治疗方案设计中，以 Efgartigimod、Rozanolixizumab 和 Batoclimab 为代表的新生儿 Fc 受体抑制剂与补体和 B 细胞抑制剂药物相比，显示出最有效的应答率。

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Initiation response, maximized therapeutic efficacy, and post-treatment effects of biological targeted therapies in myasthenia gravis: a systematic review and network meta-analysis.

Background: As targeted drug development in myasthenia gravis (MG) continues to advance, it is important to compare the efficacy of these drugs for better clinical decision-making. However, due to the varied regimens and dosages used in clinical trials for different drugs, a standardized comparison between them is necessary.

Methods: This study enrolled participants in phase II and III trials of innovative targeted drugs for MG. The primary outcome was the change in Quantitative Myasthenia Gravis score (MG-QMG) from baseline. The efficacy of all drugs at four time points was separately analyzed at four time points: initiation 1 week, initiation 4 weeks, maximized response, and post last dose 4 weeks. A network meta-analysis was conducted to compare the results of the different drugs.

Results: A total of 9 drugs, including Efgartigimod, Rozanolixizumab, Batoclimab, Eculizumab, Belimumab, Zilucoplan, Ravulizumab, Nipocalimab, Rituximab, derived from 12 studies were analyzed. At the initiation 1-week time point, three drugs exhibited significant improvement compared to the placebo effect: Efgartigimod, Zilucoplan, Rozanolixizumab. At the initiation 4-week time point, four drugs showed significant improvement compared to the placebo effect: Efgartigimod, Rozanolixizumab, Batoclimab, Zilucoplan. At the maximized response time point, six drugs achieved significant improvement compared to the placebo effect: Efgartigimod, Rozanolixizumab, Batoclimab, Eculizumab, Zilucoplan, Ravulizumab. At the post last dose 4-week point, all drugs statistically showed no significant difference from the placebo.

Conclusion: Although the MG subtypes were not consistent across trials, within the regimen design of each trial, neonatal Fc receptor inhibitors-represented by Efgartigimod, Rozanolixizumab, and Batoclimab-exhibited the most effective response rates when compared to complement and B-cell inhibitor drugs.

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来源期刊

Frontiers in Neurology CLINICAL NEUROLOGYNEUROSCIENCES -NEUROSCIENCES

CiteScore

4.90

自引率

8.80%

发文量

2792

审稿时长

14 weeks

期刊介绍： The section Stroke aims to quickly and accurately publish important experimental, translational and clinical studies, and reviews that contribute to the knowledge of stroke, its causes, manifestations, diagnosis, and management.