蛋白质组学中节律性变异对统计能力和生物标志物鉴定的挑战和机遇。

npj Biological Timing and Sleep Pub Date : 2025-01-01 Epub Date: 2025-01-25 DOI:10.1038/s44323-024-00020-2
Matt Spick, Cheryl M Isherwood, Lee A Gethings, Christopher J Hughes, Matthew E Daly, Hana Hassanin, Daan R van der Veen, Debra J Skene, Jonathan D Johnston
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引用次数: 0

摘要

生物流体和组织的分子谱在一天中的时间变化是一个很好的描述现象,但是,特别是对于蛋白质组学来说,很少考虑到这对可重复的生物标志物鉴定提出的挑战。我们提供了人类昼夜节律和蛋白质的超节律性的案例研究分析,包括补体和凝血级联以及载脂蛋白,其中PLG, CFAH, ZA2G和ITIH2首次被证明是有节律的。我们还表明,由于方差增加导致统计能力降低,节律性增加了II型错误的风险,并且控制有节奏的时间变化提高了统计能力并减少了II型错误的机会。我们建议蛋白质组学研究设计的最佳实践应考虑到时间变化,并将采样时间作为研究元数据的一部分进行报告。这些简单的步骤可以减少错误和遗漏的发现,并提高可重复性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Challenges and opportunities for statistical power and biomarker identification arising from rhythmic variation in proteomics.

Time-of-day variation in the molecular profile of biofluids and tissues is a well-described phenomenon, but-especially for proteomics-is rarely considered in terms of the challenges this presents to reproducible biomarker identification. We provide a case study analysis of human circadian and ultradian rhythmicity in proteins, including in the complement and coagulation cascades and apolipoproteins, with PLG, CFAH, ZA2G and ITIH2 demonstrated as rhythmic for the first time. We also show that rhythmicity increases the risk of Type II errors due to the reduction in statistical power from increased variance, and that controlling for rhythmic time-of-day variation improves statistical power and reduces the chances of Type II errors. We recommend that best practice in proteomics study design should account for temporal variation and that time of sampling be reported as part of study metadata. These simple steps can mitigate against both false and missed discoveries, as well as improving reproducibility.

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