Jiang Fan, Zhang Fenghe, Su Yue, Zhang Chao, Chang Ting
Department of Neurology, Tangdu Hospital, The Fourth Military Medical University, Xi'an, China.
Section of Health, No. 94804 Unit of the Chinese People's Liberation Army, Shanghai, 200434, China.
Heliyon. 2024 May 31;10(11):e31744. doi: 10.1016/j.heliyon.2024.e31744. eCollection 2024 Jun 15.
BACKGROUND: Multiple sclerosis (MS) is a heterogeneous autoimmune disease, with a rapidly evolving body of literature on disease-modifying therapy (DMT) that urgently needs to be synthesized and regularized. METHODS: The original material used for the analysis was obtained from the Web of Science Core Collection (WoSCC) in the Science Citation Index Expanded Edition (SCI-E). The data material was accessed through VOSviewer, Citespace, R package "Bibliometrix", and Scimago Graphica for data analysis and visualization. Among them, the clustering algorithm based on the Largest Likelihood Ratio (LLR) and the burst citation algorithm is the key. RESULTS: As of November 6th, 2022, 4142 publications related to emerging disease-modifying therapies (e-DMT) for MS, 6521 publications related to traditional disease-modifying therapies (t-DMT) for MS, and 1793 publications in cross-cutting disease-modifying therapies (I-DMT) for MS were included in the analysis, respectively. Publications related to DMT in MS were analyzed descriptively (for three subjects: country, institution, and author) and predictively (for two subjects: keywords and references) separately according to three sections: e-DMT, t-DMT, and I-DMT. Topics that still have relevant reference output as of 2022 include the safety of Coronavirus disease 2019 (COVID-19) mRNA vaccination, therapeutic inertia (TI), cladribine tablets, autologous hematopoietic stem cell transplantation (aHSCT), progressive multiple sclerosis, and pediatric multiple sclerosis. CONCLUSION: The future research focus for MS DMT is the combination trial or cross-trial of various treatment methods to improve the development of individualized treatment plans for MS patients. The exact contents of the research frontiers are included but not limited to ocrelizumab, fingolimod and other monoclonal antibodies, fumaric acid ester, cladribine tablet, aHSCT, and other interventions of randomized controlled trials (RCTs); the impact of mRNA COVID-19 vaccination on MS patients; TI, patient adherence, and other medical management issues; and continued exploration of biomarkers for more accurate disease classification based on the existing clinical indication classification.
背景:多发性硬化症(MS)是一种异质性自身免疫性疾病,关于疾病修正疗法(DMT)的文献迅速增加,迫切需要进行综合和规范。 方法:用于分析的原始材料来自科学引文索引扩展版(SCI-E)中的科学网核心合集(WoSCC)。通过VOSviewer、Citespace、R包“Bibliometrix”和Scimago Graphica对数据材料进行数据分析和可视化。其中,基于最大似然比(LLR)的聚类算法和突发引用算法是关键。 结果:截至2022年11月6日,分析分别纳入了4142篇与MS新兴疾病修正疗法(e-DMT)相关的出版物、6521篇与MS传统疾病修正疗法(t-DMT)相关的出版物以及1793篇与MS交叉疾病修正疗法(I-DMT)相关的出版物。根据e-DMT、t-DMT和I-DMT三个部分,分别对MS中与DMT相关的出版物进行描述性分析(针对国家、机构和作者三个主题)和预测性分析(针对关键词和参考文献两个主题)。截至2022年仍有相关参考文献产出的主题包括2019冠状病毒病(COVID-19)mRNA疫苗接种的安全性、治疗惰性(TI)、克拉屈滨片、自体造血干细胞移植(aHSCT)、进行性多发性硬化症和儿童多发性硬化症。 结论:MS DMT未来的研究重点是各种治疗方法的联合试验或交叉试验,以促进MS患者个体化治疗方案的制定。研究前沿的确切内容包括但不限于奥瑞珠单抗、芬戈莫德等单克隆抗体、富马酸酯、克拉屈滨片、aHSCT以及其他随机对照试验(RCT)干预措施;mRNA COVID-19疫苗接种对MS患者的影响;TI、患者依从性等医疗管理问题;以及基于现有临床指征分类继续探索生物标志物以进行更准确的疾病分类。
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