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Time-series modeling of multiple sclerosis disease activity: A promising window on disease progression and repair potential?

机译:多发性硬化症疾病活动的时间序列建模:疾病进展和修复潜力的有希望的窗口?

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摘要

This article discusses and reviews advanced forms of serial morphometry in the context of a disease progression model in multiple sclerosis (MS). This model of disease activity distinguishes between overall disease activity and the proportion thereof that becomes permanent damage. This translates into a progression model that features a , which, when exhausted, marks the conversion or progression from relapsing to progressive disease. The level of repair capacity at a given time determines the rate of progression. Both clinical and MRI variables appear to be in support of such a model. We examine possible MRI markers for this repair capacity, particularly the short-term behavior of new MRI lesions, quantified by methods of time-series analysis—that is, capturing lesion dynamics in the form of MRI intensity change directly, rather than shape or volume change. Lower rates of individual lesion recovery may represent lower repair and greater proximity to a progressive stage. Individuals with low transient lesion turnover appear to undergo more rapid progression and atrophy. Because disease-modifying therapies aim to alter the pathophysiological chain of inflammation, demyelination, and axonal loss, a therapeutic effect may therefore be more readily apparent as a change in lesion dynamics and recovery rate and level, rather than a change in total lesion burden or enhancing lesion number.
机译:本文在多发性硬化症(MS)中的疾病进展模型的背景下讨论和评论先进形式的连续形态。这种疾病活动模型区分了整体疾病活动和变得永久性损伤的比例。这转化为一个渐进模型,其特征在于,它在耗尽时,将转换或进展标记对渐进性疾病。给定时间的修复能力水平决定了进展速率。临床和MRI变量都似乎可以支持这种模型。我们检查这种修复能力的可能MRI标记,特别是通过时间序列分析方法量化的新MRI病变的短期行为 - 即,捕获MRI强度的形式直接捕获病变动态,而不是形状或体积改变。单个病变恢复的较低率可以代表更低的修复和更高的渐进阶段。瞬态病变营业额低的个体似乎经历了更快的进展和萎缩。由于疾病改性疗法的目的是改变炎症,脱髓鞘和轴突损失的病理生理链,因此可以更加明显地显而易见,因为病变动力学和恢复率和水平的变化,而不是总病变负担的变化或增强病变数。

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