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液体生物样本库分析前工作流程的质量评估:牛磺酸作为分析前过程变异的血清特异性质量指标

Quality Assessment of the Preanalytical Workflow in Liquid Biobanking: Taurine as a Serum-Specific Quality Indicator for Preanalytical Process Variations.

作者信息

Schwarz Nicolle, Knutti Nadine, Rose Michael, Neugebauer Sophie, Geiger Jörg, Jahns Roland, Klopp Norman, Illig Thomas, Mathay Conny, Betsou Fay, Scherag André, Kiehntopf Michael

机构信息

Institute of Clinical Chemistry and Laboratory Diagnostics and Integrated Biobank Jena (IBBJ), Jena University Hospital, Jena, Germany.

Interdisciplinary Bank of Biomaterials and Data Würzburg (ibdw), Würzburg, Germany.

出版信息

Biopreserv Biobank. 2019 Oct;17(5):458-467. doi: 10.1089/bio.2019.0004. Epub 2019 Jul 24.

Abstract

The scientific impact of translational biomedical research largely depends on the availability of high-quality biomaterials. However, evidence-based and robust quality indicators (QIs) covering the most relevant preanalytical variations are still lacking. The aim of this study was to identify and validate a QI suitable for assessing time-to-centrifugation (TTC) delays in human liquid biospecimens originating from both healthy and diseased individuals. Serum and plasma samples with varying TTCs were analyzed by liquid chromatography coupled to tandem mass spectrometry (LC-MS/MS) in a pilot cohort of healthy individuals to identify a suitable QI candidate. Taurine (TAU), as a TTC QI candidate, was validated in healthy individuals and patients with rheumatologic and cardiologic diseases, considering the (1) preanalytical handling temperature, (2) platelet count, and (3) postcentrifugation delay. For discrimination of high TTC (TTC >60 minutes) from low TTC serum specimens, a probability calculation tool was developed (Triple-T-cutoff-model). TTC-dependent changes in healthy individuals were observed for amino acids, particularly TAU. Validation of the TAU levels in an independent cohort of healthy individuals revealed a time-dependent increase in serum, but not in plasma, for a TTC delay of 30-240 minutes. TAU increases were dependent on the handling temperature and platelet count and volume. By contrast, no changes in TAU concentrations were observed for additional postcentrifugation delays. Validation of TAU and the Triple-T-cutoff-model, in rheumatologic/cardiologic patient collectives, allowed the discrimination of samples with TTC ≤60 min/>60 min with estimated AUROC (area under the receiver operating characteristic curve) values of 89% [78%-100%]/86% [71%-100%] and 91% [79%-100%]/84% [68%-100%], respectively. Considering the preanalytical handling temperature and platelet count and volume, TAU and the Triple-T-cutoff-model represent reliable QIs for TTC >60 minutes in serum samples from healthy individuals and selected rheumatologic/cardiologic patients. However, further studies in larger patient collectives with various diseases are needed to assess the robustness and potential of the QIs presented in this article as biobanking quality assurance/quality control tools to support high-quality biomedical research.

摘要

转化性生物医学研究的科学影响力在很大程度上取决于高质量生物材料的可获得性。然而,涵盖最相关分析前变异的基于证据且可靠的质量指标(QIs)仍然缺乏。本研究的目的是识别并验证一个适用于评估来自健康个体和患病个体的人体液体生物样本离心时间(TTC)延迟的质量指标。在一组健康个体的试点队列中,通过液相色谱-串联质谱(LC-MS/MS)分析了具有不同TTC的血清和血浆样本,以确定一个合适的质量指标候选物。考虑到(1)分析前处理温度、(2)血小板计数和(3)离心后延迟,牛磺酸(TAU)作为TTC质量指标候选物,在健康个体以及患有风湿病和心脏病的患者中进行了验证。为了区分高TTC(TTC>60分钟)和低TTC血清样本,开发了一种概率计算工具(Triple-T截止模型)。在健康个体中观察到氨基酸尤其是TAU随TTC的变化。在一组独立的健康个体中对TAU水平进行验证发现,对于30 - 240分钟的TTC延迟,血清中TAU水平呈时间依赖性增加,而血浆中未观察到这种情况。TAU的增加取决于处理温度、血小板计数和体积。相比之下,对于额外的离心后延迟,未观察到TAU浓度的变化。在风湿病/心脏病患者群体中对TAU和Triple-T截止模型进行验证,能够区分TTC≤60分钟/>60分钟的样本,估计的受试者操作特征曲线下面积(AUROC)值分别为89% [78% - 100%]/86% [71% - 100%]和91% [79% - 100%]/84% [68% - 100%]。考虑到分析前处理温度、血小板计数和体积,TAU和Triple-T截止模型是健康个体和选定的风湿病/心脏病患者血清样本中TTC>6分钟的可靠质量指标。然而,需要在更大的患有各种疾病的患者群体中进行进一步研究,以评估本文提出的质量指标作为生物样本库质量保证/质量控制工具支持高质量生物医学研究的稳健性和潜力。

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