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全自动校正非容量干血斑磷脂酰乙醇分析的血细胞比容偏倚。

Fully automated correction for the hematocrit bias of non-volumetric dried blood spot phosphatidylethanol analysis.

机构信息

CAMAG DBS Laboratory, Sonnenmattstrasse 11, 4132 Muttenz, Switzerland.

Institute of Forensic Medicine Bern, University of Bern, Bühlstrasse 20, 3012 Bern, Switzerland.

出版信息

Alcohol. 2021 Aug;94:17-23. doi: 10.1016/j.alcohol.2021.04.002. Epub 2021 Apr 16.

DOI:10.1016/j.alcohol.2021.04.002
PMID:33865941
Abstract

The quantitative analysis of substances in dried blood spots (DBS) has gained vast popularity in the past decade. The World Anti-Doping Agency (WADA) also recently committed to implementing DBS. Currently, DBS sampling mainly has focused on various volumetric sampling devices such as Hemaxis, Capitainer, and Mitra. These devices are designed to collect a specific sample volume, independent of the hematocrit (HCT), to enable quantitative DBS analysis. Here, we present an automated solution that makes the necessity of volumetric sampling for quantitative DBS analysis obsolete. Combining automated reflectance-based HCT correction in combination with fully automated DBS LC-MS/MS analysis, the novel strategy permits high-throughput analysis in combination with HCT independence. Studying the model compound phosphatidylethanol 16:0/18:1, which is HCT-dependent due to incorporation into red blood cells, an implementation of DBS HCT normalization is presented. First, the performance of the automated HCT module with DBS is demonstrated compared to standardized HCT analysis from whole blood using a centrifuge. Second, the HCT dependency of fully automated PEth analysis from DBS is evaluated. Third, a solution to correct for the HCT dependency of PEth using the HCT scanner is presented. The study demonstrates that as soon as the HCT dependence of an analyte is known, a correction factor can be applied for the normalization of HCT levels. In the context of PEth, a linear increase in PEth concentration was observed, as the analyte is primarily located within the cellular fraction. Based on the obtained results, the use of a common correction factor for PEth DBS is possible.

摘要

过去十年中,干血斑(DBS)中物质的定量分析得到了广泛的关注。世界反兴奋剂机构(WADA)最近也承诺实施 DBS。目前,DBS 采样主要集中在各种体积采样设备上,如 Hemaxis、Capitainer 和 Mitra。这些设备旨在采集特定的样本体积,与红细胞压积(HCT)无关,以实现定量 DBS 分析。在这里,我们提出了一种自动化解决方案,使定量 DBS 分析的体积采样变得不必要。通过将基于自动反射的 HCT 校正与全自动 DBS LC-MS/MS 分析相结合,这种新策略允许与 HCT 无关的高通量分析。通过研究由于掺入红细胞而与 HCT 相关的模型化合物磷脂酰乙醇 16:0/18:1,提出了一种 DBS HCT 归一化的实现方法。首先,将基于自动化 HCT 模块的 DBS 与使用离心机的标准化全血 HCT 分析进行比较,以验证其性能。其次,评估了从 DBS 进行全自动 PEth 分析的 HCT 依赖性。第三,提出了一种使用 HCT 扫描仪校正 PEth 的 HCT 依赖性的解决方案。该研究表明,只要分析物的 HCT 依赖性已知,就可以应用校正因子来归一化 HCT 水平。在 PEth 的情况下,观察到 PEth 浓度的线性增加,因为分析物主要位于细胞部分。基于所获得的结果,对于 PEth DBS,可以使用通用的校正因子。

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