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两种快速、准确的液相色谱串联质谱法用于定量七种尿毒症毒素:在急性肾损伤背景下描述其蓄积动力学特征的应用。

Two rapid, accurate liquid chromatography tandem mass spectrometry methods for the quantification of seven uremic toxins: An application for describing their accumulation kinetic profile in a context of acute kidney injury.

作者信息

André Camille, Bennis Youssef, Titeca-Beauport Dimitri, Caillard Pauline, Cluet Yan, Kamel Said, Choukroun Gabriel, Maizel Julien, Liabeuf Sophie, Bodeau Sandra

机构信息

EA 7517 MP3CV, UPJV, F-80054 Amiens, France; Laboratory of Pharmacology and Toxicology, Amiens-Picardie University Hospital, F-80054 Amiens, France.

EA 7517 MP3CV, UPJV, F-80054 Amiens, France; Department of Nephrology Dialysis and Transplantation, Amiens-Picardie University Hospital, F-80054 Amiens, France; Department of Medical Intensive Care, Amiens-Picardie University Hospital, F-80054 Amiens, France.

出版信息

J Chromatogr B Analyt Technol Biomed Life Sci. 2020 Sep 1;1152:122234. doi: 10.1016/j.jchromb.2020.122234. Epub 2020 Jun 13.

Abstract

Acute kidney injury (AKI) is a frequent, serious complication in critically ill patients. Even if renal replacement therapy is rapidly initiated, AKI may lead to the acute accumulation of metabolic waste products called uremic toxins (UTs). Although the accumulation and effects of UTs have been extensively described in the setting of chronic kidney disease (CKD), few data are available for AKI. A rapid, sensitive, specific method with simple sample preparation is required to facilitate routine blood monitoring of UTs in a context of acute accumulation. We have developed and validated two fast liquid chromatography tandem mass spectrometry methods for the quantification of seven UTs in human serum. The first method (in negative ionization mode) enables the quantification of five UTs (hippuric acid (HA), indoxyl sulfate (IxS), para-cresyl sulfate (pCS), para-cresyl glucuronide (pCG), 3-carboxy-4-methyl-5-propyl-2-furanpropionate (CMPF)). The second method (in positive ionization mode) enables the quantification of two UTs (indole-3-acetic acid (IAA), and trimethylamine N-oxide (TMAO)). Sample preparation consisted of the deproteinization of a small volume of serum (50 µL). The run-times required to assay all the UTs in negative and positive ionization modes were only 2.5 and 2 min, respectively. In order to obtain a reliable, toxin-free matrix for the preparation of calibration standards and quality controls, serum was pretreated with activated charcoal. We used these methods to determine the time course of UT accumulation in eight patients who developed an AKI after cardiac surgery. The calibration curves ranged from 0.1 to 100 µg mL for all the UTs (except for IAA: 0.5 to 100 µg mL), and the correlation coefficients were above 0.999 for all. The methods were reproducible, repeatable, and accurate, with all coefficients of variation and biases below 15%. The highest concentrations measured in patients with AKI were lower than those reported in CKD stages 4 and 5 but higher than those observed in patients with no impairment of renal function (particularly for IxS and pCS). Our results also highlighted low accumulation of the other toxins (IAA, HA, TMAO, pCG, and CMPF). The UT concentrations did not rise earlier than that of creatinine; although the return to baseline took longer than for creatinine for some compounds. Lastly, assessment of the time course of UT accumulation as a prognostic marker for AKI (particularly for pCS and IxS) appears to be promising and should be continued in a larger number of patients.

摘要

急性肾损伤(AKI)是危重症患者常见的严重并发症。即便迅速启动肾脏替代治疗,AKI仍可能导致称为尿毒症毒素(UTs)的代谢废物急性蓄积。尽管UTs的蓄积及其影响在慢性肾脏病(CKD)背景下已有广泛描述,但关于AKI的相关数据却很少。需要一种快速、灵敏、特异且样品制备简单的方法,以方便在急性蓄积情况下对UTs进行常规血液监测。我们已开发并验证了两种快速液相色谱串联质谱法,用于定量人血清中的七种UTs。第一种方法(负离子化模式)可定量五种UTs(马尿酸(HA)、硫酸吲哚酚(IxS)、对甲酚硫酸酯(pCS)、对甲酚葡萄糖醛酸苷(pCG)、3-羧基-4-甲基-5-丙基-2-呋喃丙酸(CMPF))。第二种方法(正离子化模式)可定量两种UTs(吲哚-3-乙酸(IAA)和氧化三甲胺(TMAO))。样品制备包括对少量血清(50 μL)进行脱蛋白处理。在负离子化和正离子化模式下测定所有UTs所需的运行时间分别仅为2.5分钟和2分钟。为了获得用于制备校准标准品和质量控制品的可靠、无毒素基质,血清用活性炭进行了预处理。我们使用这些方法来确定八名心脏手术后发生AKI的患者中UTs蓄积的时间进程。所有UTs的校准曲线范围为0.1至100 μg/mL(IAA除外:0.5至100 μg/mL),且所有相关系数均高于0.999。这些方法具有可重复性、可再现性和准确性,所有变异系数和偏差均低于15%。AKI患者中测得的最高浓度低于CKD 4期和5期报告的浓度,但高于肾功能无损害患者中观察到的浓度(特别是IxS和pCS)。我们的结果还突出显示了其他毒素(IAA、HA、TMAO、pCG和CMPF)的低蓄积情况。UTs浓度升高的时间不早于肌酐;尽管某些化合物恢复至基线的时间比肌酐更长。最后,将UTs蓄积的时间进程评估为AKI的预后标志物(特别是对于pCS和IxS)似乎很有前景,应在更多患者中继续进行研究。

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