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理解多发性硬化症作为一种疾病谱:临床阈值以上和以下。

Understanding multiple sclerosis as a disease spectrum: above and below the clinical threshold.

机构信息

Corinne Goldsmith Dickinson Center for MS, Icahn School of Medicine at Mount Sinai.

Medical Education Director, Neurology at Heartbeat/Publicis Health, New York.

出版信息

Curr Opin Neurol. 2024 Jun 1;37(3):189-201. doi: 10.1097/WCO.0000000000001262. Epub 2024 Apr 9.

Abstract

PURPOSE OF REVIEW

Research in multiple sclerosis (MS) has long been predicated on clinical groupings that do not reflect the underlying biologic heterogeneity apparent within patient populations. This review explicates the various levels of explanation through which the spectrum of disease is described and investigated both above and below the clinical threshold of detection, as framed by the topographical model of MS, to help advance a cogent mechanistic framework.

RECENT FINDINGS

Contemporary evidence has amended the view of MS as consisting of sequential disease phases in favor of a spectrum of disease with an admixture of interdependent and dynamic pathobiological axes driving tissue injury and progression. Recent studies have shown the presence of acute and compartmentalized inflammation and mechanisms of neurodegeneration beginning early and evolving throughout the disease continuum. Still, the gap between the understanding of immunopathologic processes in MS and the tools used to measure relevant molecular, laboratory, radiologic, and clinical metrics needs attention to enable better prognostication of disease and monitoring for changes along specific pathologic axes and variable treatment outcomes.

SUMMARY

Aligning on a consistently-applied mechanistic framework at distinct levels of explanation will enable greater precision across bench and clinical research, and inform discourse on drivers of disability progression and delivery of care for individuals with MS.

摘要

目的综述: 长期以来,多发性硬化症(MS)的研究一直基于临床分组,而这些分组并不能反映患者群体中明显存在的潜在生物学异质性。本综述详细说明了通过多种解释层次来描述疾病谱的方法,这些解释层次既包括在临床检测阈值以上和以下的描述,也包括 MS 地形学模型所框定的检测,以帮助推进一个有说服力的机制框架。

最近的发现: 目前的证据修正了 MS 由连续疾病阶段组成的观点,转而支持疾病谱的概念,其中混合了相互依赖和动态的病理生物学轴,这些轴驱动着组织损伤和进展。最近的研究表明,急性和隔室性炎症以及神经退行性变的机制早在疾病连续体中就已经存在,并不断演变。尽管如此,在 MS 中免疫病理过程的理解与用于测量相关分子、实验室、影像学和临床指标的工具之间仍存在差距,需要加以关注,以便更好地预测疾病,并监测特定病理轴和可变治疗结果的变化。

总结: 在不同的解释层次上达成一致的应用机制框架,将使临床前和临床研究更加精确,并为残疾进展的驱动因素和 MS 患者的护理提供信息。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7389/11064902/f8b68c93bf4e/coneu-37-189-g001.jpg

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