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HNE与组氨酸及含组氨酸的肽形成迈克尔加成物,作为尿液中脂质衍生羰基应激的生物标志物:Zucker肥胖大鼠的液相色谱-串联质谱分析

HNE Michael adducts to histidine and histidine-containing peptides as biomarkers of lipid-derived carbonyl stress in urines: LC-MS/MS profiling in Zucker obese rats.

作者信息

Orioli Marica, Aldini Giancarlo, Benfatto Maria Carmela, Facino Roberto Maffei, Carini Marina

机构信息

Istituto di Chimica Farmaceutica e Tossicologica "Pietro Pratesi", Faculty of Pharmacy, University of Milan, Via Mangiagalli 25, I-20133 Milan, Italy.

出版信息

Anal Chem. 2007 Dec 1;79(23):9174-84. doi: 10.1021/ac7016184. Epub 2007 Nov 3.

Abstract

A new liquid chromatography-tandem mass spectrometric (LC-MS/MS) approach, based on the precursor ion scanning technique using a triple-stage quadrupole, has been developed to detect free and protein-bound histidine (His) residues modified by reactive carbonyl species (RCS) generated by lipid peroxidation. This approach has been applied to urines from Zucker obese rats, a nondiabetic animal model characterized by obesity and hyperlipidemia, where RCS formation plays a key role in the development of renal and cardiac dysfunction. The immonium ion of His at m/z 110 was used as a specific product ion of His-containing peptides to generate precursor ion spectra, followed by MS2 acquisitions of each precursor ion of interest for structural characterization. By this approach, three novel adducts, which are excreted in free form only, have been identified, two of them originating from the conjugation of 4-hydroxy-trans-2-nonenal (HNE) to His, followed by reduction/oxidation of the aldehyde: His-1,4-dihydroxynonane (His-DHN), His-4-hydroxynonanoic acid (His-HNA), and carnosine-HNE, this last recognized in previous in vitro studies as a new potential biomarker of carbonyl stress. No free His-HNE was found in urines, which was detected only in protein hydrolysates. The same LC-MS/MS method, working in multiple reaction monitoring (MRM) mode, has been developed, validated, and applied to quantitatively profile in Zucker urines both conventional (1,4-dihydroxynonane mercapturic acid, DHN-MA) and the newly identified adducts, except His-HNA. The analytes were separated on a C12 reversed-phase column by gradient elution from 100% A (water containing 5 mM nonafluoropentanoic acid) to 80% B (acetonitrile) in 24 min at a flow rate of 0.2 mL/min and analyzed for quantification in MRM mode by applying the following precursor-to-product ion transitions m/z 322.2 --> 164.1 + 130.1 (DHN-MA), m/z 314.7 --> 268.2 + 110.1 (His-DHN), m/z 312.2 --> 110.1 + 156.0 (His-HNE), m/z 383.1 --> 266.2 + 110.1 (CAR-HNE), m/z 319.2 --> 301.6 + 156.5 (H-Tyr-His-OH, internal standard). Precision and accuracy data, as well as the lower limits of quantification in urine, were highly satisfactory (from 0.01 nmol/mL for CAR-HNE, His-DHN, His-HNE, to 0.075 nmol/mL for DHN-MA). The method, applied to evaluate for the first time the advanced lipoxidation end products profile in urine from obese Zucker rats, an animal model for the metabolic syndrome, has proved to be suitable and sensitive enough for testing in vivo the carbonyl quenching ability of newly developed RCS sequestering agents.

摘要

一种基于使用三级四极杆的前体离子扫描技术的新型液相色谱-串联质谱(LC-MS/MS)方法已被开发出来,用于检测由脂质过氧化产生的活性羰基物质(RCS)修饰的游离和与蛋白质结合的组氨酸(His)残基。该方法已应用于Zucker肥胖大鼠的尿液,这是一种以肥胖和高脂血症为特征的非糖尿病动物模型,其中RCS的形成在肾脏和心脏功能障碍的发展中起关键作用。His在m/z 110处的亚铵离子被用作含His肽段的特定产物离子,以生成前体离子谱,随后对每个感兴趣的前体离子进行MS2采集以进行结构表征。通过这种方法,已鉴定出三种仅以游离形式排泄的新型加合物,其中两种源自4-羟基反式-2-壬烯醛(HNE)与His的共轭,随后醛发生还原/氧化:His-1,4-二羟基壬烷(His-DHN)、His-4-羟基壬酸(His-HNA)和肌肽-HNE,最后一种在先前的体外研究中被认为是羰基应激的一种新的潜在生物标志物。在尿液中未发现游离的His-HNE,仅在蛋白质水解物中检测到。同样的LC-MS/MS方法,以多反应监测(MRM)模式运行,已被开发、验证并应用于定量分析Zucker尿液中的常规加合物(1,4-二羟基壬烷巯基尿酸,DHN-MA)和新鉴定的加合物,但不包括His-HNA。分析物在C12反相柱上通过梯度洗脱进行分离,在24分钟内从100%A(含5 mM全氟戊酸的水)到80%B(乙腈),流速为0.2 mL/min,并通过应用以下前体-产物离子跃迁在MRM模式下进行定量分析:m/z 322.2 --> 164.1 + 130.1(DHN-MA)、m/z 314.7 --> 268.2 + 110.1(His-DHN)、m/z 312.2 --> 110.1 + 156.0(His-HNE)、m/z 383.1 --> 266.2 + 110.1(CAR-HNE)、m/z 319.2 --> 301.6 + 156.5(H-Tyr-His-OH,内标)。精密度和准确度数据以及尿液中的定量下限非常令人满意(CAR-HNE、His-DHN、His-HNE为0.01 nmol/mL,DHN-MA为0.075 nmol/mL)。该方法首次应用于评估肥胖Zucker大鼠(一种代谢综合征动物模型)尿液中的晚期脂质氧化终产物谱,已被证明适用于并足够灵敏,可用于体内测试新开发的RCS螯合剂的羰基淬灭能力。

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