Wilcoxon-Mann-Whitney 优势比：序数结果的统计度量，例如 EDSS,Multiple Sclerosis and Related Disorders

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Wilcoxon-Mann-Whitney 优势比：序数结果的统计度量，例如 EDSS
Multiple Sclerosis and Related Disorders ( IF 2.9 ) Pub Date : 2022-01-10 , DOI: 10.1016/j.msard.2022.103516
C W Howard ₁ , G Zou ₂ , S A Morrow ₃ , S Fridman ₃ , J M Racosta ₄

Affiliation

背景

在许多临床情况下，序数量表提供了半量化患者结果的主要方法。在多发性硬化症领域，主要的顺序量表是扩展的残疾状态量表。序数尺度统计分析的主要方法提供没有影响大小的 p 值或严重依赖赔率的比例假设，使它们缺乏力量和错误。Wilcoxon-Manny-Whitney Odds 是一种统计方法，可提供重要信息，例如 p 值、效应大小、需要治疗的数量、置信区间，并且在很大程度上没有假设。然而，它的效用尚未在多发性硬化症领域得到证实。

方法

选择了多发性硬化症领域的三项临床研究，这些研究利用了组或个体水平的序数量表结果。使用 WebPlotDigitizer 提取这些研究的数据，并将定制的 Wilxocon-Mann-Whitney Odds 软件应用于每个数据集，以重新分析研究的主要结果。

结果

Muraro 等人在 2017 年对手稿的重新分析表明，自体干细胞移植治疗复发缓解型多发性硬化症有 65% 的机会从任何扩展残疾状态量表类别中改善，尽管并不显着。Songthammawat 等人在 2019 年对手稿的重新分析表明，静脉注射甲基强的松龙和同时进行血浆置换的改善机会为 185%，而静脉注射甲基强的松龙联合血浆置换的改善机会为 32%，尽管并不显着。关于- Kister et al., 2012 的分析表明，每 5 年的研究增量，流动性或认知评分的机会普遍倾向于下降，尽管具有统计学意义，但这些效应量较小，从 11% 的改善机会到 66% 5 年间隔内下降的可能性百分比。

讨论

Wilcoxon-Mann-Whitney Odds 凭借其稳健的基本无假设性质简化了序数数据分析。代替许多统计检验，这个单一检验提供效应大小估计、需要治疗的数量、p 值和置信区间。重要的是，Wilcoxon-Mann-Whitney Odds 效应大小计算直观地适用于个人和人口水平。此外，Wilcoxon-Mann-Whitney Odds 可以直观地描述大型队列随时间的进展，并且我们能够清楚地传达大型多发性硬化症队列 30 年内流动性和认知能力下降的几率。总体而言，Wilcoxon-Mann-Whitney Odds 是一项功能强大且稳健的统计检验，在多发性硬化症领域具有重大前景。

"点击查看英文标题和摘要"

Wilcoxon-Mann-Whitney odds ratio: A statistical measure for ordinal outcomes such as EDSS

Background

In many clinical situations, ordinal scales afford the primary method of semi-quantifying patient outcomes. In the field of multiple sclerosis, the primary ordinal scale is the Expanded Disability Status Scale. Predominant methods of ordinal scale statistical analysis provide a p-value without effect size or rely heavily on the assumption of proportionality of odds, subjecting them to lack of power and error. The Wilcoxon-Manny-Whitney Odds is a statistical method which provides significant information such as p-value, effect size, number needed to treat, confidence intervals, and is largely assumption-free. However, its utility has not been demonstrated in the field of multiple sclerosis.

Methods

Three clinical studies in the field of multiple sclerosis were selected which utilized ordinal scale outcomes at group or individual levels. Data from these studies was extracted using WebPlotDigitizer, and a custom Wilxocon-Mann-Whitney Odds software was applied to each dataset to re-analyze the main outcomes of the studies.

Results

Re-analysis of the manuscript by Muraro et al., 2017 demonstrated that autologous stem cell transplantation for relapsing remitting multiple sclerosis resulted in a 65% chance of improving from any Expanded Disability Status Scale category, although not significant. Re-analysis of the manuscript by Songthammawat et al., 2019 demonstrated chance of improvement with intravenous methylprednisolone and concurrent plasma exchange was 185% versus 32% in intravenous methylprednisolone with add-on plasma exchange, although not significant. Re-analysis of Kister et al., 2012 demonstrated the chances of mobility or cognition scores generally favored decline at every 5-year increment of study, and although statistically significant, these were smaller effect sizes ranging from an 11% chance of improvement to a 66% chance of decline over a 5-year interval.

Discussion

The Wilcoxon-Mann-Whitney Odds simplifies ordinal data analysis with its robust largely assumption-free nature. In the place of numerous statistical tests, this single test provides effect size estimate, number needed to treat, p-values, and confidence intervals. Importantly, the Wilcoxon-Mann-Whitney Odds effect size calculation is intuitively applicable to both individual and population-levels. Further, the Wilcoxon-Mann-Whitney Odds allows intuitive description of the progression of large cohorts over time, and we were able to clearly convey the odds of mobility and cognitive decline over 30 years in a large multiple sclerosis cohort. Overall, the Wilcoxon-Mann-Whitney Odds is a powerful and robust statistical test with significant promise within the field of multiple sclerosis.

更新日期：2022-02-02

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