Using differential mobility spectrometry to improve the specificity of targeted measurements of 2,3-dinor 11β-Prostaglandin F2α

IF 2.5 3区 医学 Q2 MEDICAL LABORATORY TECHNOLOGY Clinical biochemistry Pub Date : 2024-03-08 DOI:10.1016/j.clinbiochem.2024.110745
Kayla Moehnke, Jennifer Kemp, Michelle R. Campbell, Ravinder J. Singh, Anne E. Tebo, Anthony Maus
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Abstract

Introduction

2,3-dinor 11β-Prostaglandin F2α (BPG) is an arachidonic acid derivative and the most abundant metabolic byproduct of prostaglandin D2, which is released during mast cell activation. Therefore, measurements of BPG in urine using liquid chromatography-tandem mass spectrometry (LC-MS/MS) provide a noninvasive method for evaluation and management of mast cell disorders. Measurements obtained by LC-MS/MS exhibit a high prevalence of chromatographic interferences resulting in challenges with optimal determination of BGP. In this investigation, differential mobility spectrometry (DMS) is utilized to overcome the limitations of current testing.

Methods

Urine samples were extracted using an automated solid-phase extraction method. Samples were then analyzed with and without DMS devices installed on two commercially available mass spectrometry platforms to assess the benefits of DMS. Following promising results from a preliminary analytical evaluation, LC-DMS-MS/MS measurements of BPG in urine were fully validated to assess the analytical implications of using this technology.

Results and discussion

The addition of DMS devices to the LC-MS/MS systems evaluated in this investigation significantly reduced interferences observed in the chromatograms. Concomitantly, DMS reduced the number of discordant quantifier/qualifier fragment ion results that significantly exceeded the ± 20 % limits, suggesting greater analytical specificity. The validation studies yielded low interday imprecision, with %CVs less than 6.5 % across 20 replicate measurements. Validation studies assessing other aspects of analytical performance also met acceptance criteria.

Conclusions

Incorporating DMS devices greatly improved the specificity of BPG measurements by LC-MS/MS, as evidenced by the comparison of chromatograms and fragment ion results. Validation studies showed exceptional performance for established analytical metrics, indicating that this technology can be used to minimize the impact of interferences without adversely impacting other aspects of analytical or clinical performance.

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利用差示迁移率光谱法提高 2,3-dinor 11β-Prostaglandin F2α 靶向测量的特异性。
导言:2,3-dinor 11β-前列腺素 F2α(BPG)是一种花生四烯酸衍生物,也是前列腺素 D2 最丰富的代谢副产品,前列腺素 D2 在肥大细胞活化过程中释放。因此,使用液相色谱-串联质谱法(LC-MS/MS)测量尿液中的 BPG 可为肥大细胞疾病的评估和管理提供一种无创方法。液相色谱-串联质谱(LC-MS/MS)法的测量结果显示,色谱干扰非常普遍,这给最佳测定 BGP 带来了挑战。在这项研究中,差示迁移率光谱法(DMS)被用来克服目前检测方法的局限性:方法:采用自动固相萃取法提取尿样。方法:采用自动固相萃取法提取尿样,然后在两个市售质谱平台上分别安装和未安装 DMS 装置对尿样进行分析,以评估 DMS 的优势。在初步分析评估取得良好结果后,对尿液中 BPG 的 LC-DMS-MS/MS 测量进行了全面验证,以评估使用该技术的分析意义:在本次调查评估的 LC-MS/MS 系统中添加 DMS 装置可显著减少色谱图中的干扰。同时,DMS 还减少了定量/定性片段离子不一致的结果数量,这些结果明显超过了 ± 20 % 的限值,表明分析的特异性更高。验证研究得出的日间不精确度较低,20 次重复测量的 %CV 小于 6.5%。评估分析性能其他方面的验证研究也达到了验收标准:结论:通过色谱图和碎片离子结果的比较,DMS 装置大大提高了 LC-MS/MS 测量 BPG 的特异性。验证研究显示,该技术在既定的分析指标方面表现优异,表明该技术可用于最大限度地降低干扰的影响,而不会对分析或临床性能的其他方面造成不利影响。
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来源期刊
Clinical biochemistry
Clinical biochemistry 医学-医学实验技术
CiteScore
5.10
自引率
0.00%
发文量
151
审稿时长
25 days
期刊介绍: Clinical Biochemistry publishes articles relating to clinical chemistry, molecular biology and genetics, therapeutic drug monitoring and toxicology, laboratory immunology and laboratory medicine in general, with the focus on analytical and clinical investigation of laboratory tests in humans used for diagnosis, prognosis, treatment and therapy, and monitoring of disease.
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