利用替代基质法开发、验证和应用一种 LC-MS/MS 方法,以定量检测人体血浆中游离形式的微量营养素奎宁和奎宁酸。

IF 3.8 2区 化学 Q1 BIOCHEMICAL RESEARCH METHODS
Xiaobei Pan, Swathine Chandrasekaran, Jayne V Woodside, Steffi G Riedel-Heller, Martin Scherer, Michael Wagner, Alfredo Ramirez, Brian D Green
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引用次数: 0

摘要

奎奎宁(Q)是一种超模态 7-脱氮鸟苷核苷,专门由细菌合成。人类可从肠道微生物菌群或消化的食物中回收这种微量营养素及其相应的核碱基形式奎奎宁(q)。人或小鼠细胞中 Q-tRNA 的耗竭会导致蛋白质错误折叠,从而引发内质网压力和未折叠蛋白质反应的激活。在体内,这会降低小鼠大脑的神经元结构,影响学习和记忆。在此,我们开发、优化并验证了一种灵敏的方法,用于量化人体血液中的游离q和Q。在对几种不同固相吸附剂的q/Q萃取效率进行评估后,发现Bond Elut PBA(苯硼酸)滤芯对集合人体血浆中q(82%)和Q(71%)的萃取回收率最高。在方法开发和验证过程中,使用含 4% BSA 的 PBS 作为替代基质。在 0.0003-1 µM 的浓度范围内对 q 和 Q 的 LC-MS/MS 方法进行了验证,结果表明该方法具有良好的线性(r2 = 0.997 (q)和 r2 = 0.998 (Q))、定量限(0.0003 µM)、准确度(100.39-125.71%)和精密度(CV%)。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Development, validation and application of an LC-MS/MS method quantifying free forms of the micronutrients queuine and queuosine in human plasma using a surrogate matrix approach.

Development, validation and application of an LC-MS/MS method quantifying free forms of the micronutrients queuine and queuosine in human plasma using a surrogate matrix approach.

Queuosine (Q) is a hypermodified 7-deaza-guanosine nucleoside exclusively synthesized by bacteria. This micronutrient and its respective nucleobase form queuine (q) are salvaged by humans either from gut microflora or digested food. Depletion of Q-tRNA in human or mouse cells causes protein misfolding that triggers endoplasmic reticular stress and the activation of the unfolded protein responses. In vivo, this reduces the neuronal architecture of the mouse brain affecting learning and memory. Herein, a sensitive method for quantifying free q and Q in human blood was developed, optimised and validated. After evaluating q/Q extraction efficiency in several different solid-phase sorbents, Bond Elut PBA (phenylboronic acid) cartridges were found to have the highest extraction recovery for q (82%) and Q (71%) from pooled human plasma. PBS with 4% BSA was used as surrogate matrix for method development and validation. An LC-MS/MS method was validated across the concentration range of 0.0003-1 µM for both q and Q, showing excellent linearity (r2 = 0.997 (q) and r2 = 0.998 (Q)), limit of quantification (0.0003 µM), accuracy (100.39-125.71%) and precision (CV% < 15.68%). In a sampling of healthy volunteers (n = 44), there was no significant difference in q levels between male (n = 14; mean = 0.0068 µM) and female (n = 30; mean = 0.0080 µM) participants (p = 0.50). Q was not detected in human plasma. This validated method can now be used to further substantiate the role of q/Q in nutrition, physiology and pathology.

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来源期刊
CiteScore
8.00
自引率
4.70%
发文量
638
审稿时长
2.1 months
期刊介绍: Analytical and Bioanalytical Chemistry’s mission is the rapid publication of excellent and high-impact research articles on fundamental and applied topics of analytical and bioanalytical measurement science. Its scope is broad, and ranges from novel measurement platforms and their characterization to multidisciplinary approaches that effectively address important scientific problems. The Editors encourage submissions presenting innovative analytical research in concept, instrumentation, methods, and/or applications, including: mass spectrometry, spectroscopy, and electroanalysis; advanced separations; analytical strategies in “-omics” and imaging, bioanalysis, and sampling; miniaturized devices, medical diagnostics, sensors; analytical characterization of nano- and biomaterials; chemometrics and advanced data analysis.
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