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A High Resolution/Accurate Mass (HRAM) Data-Dependent MS3 Neutral Loss Screening Classification and Relative Quantitation Methodology for Carbonyl Compounds in Saliva

机译:唾液中羰基化合物的高分辨率/精确质量(HRAM)数据相关的MS3中性损失筛选分类和相对定量方法

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摘要

Reactive carbonyl compounds (RCCs) are ubiquitous in the environment and are generated endogenously as a result of various physiological and pathological processes. These compounds can react with biological molecules inducing deleterious processes believed to be at the basis of their toxic effects. Several of these compounds are considered to be implicated in neurotoxic processes, aging disorders, and cancer. Therefore, a method characterizing exposures to these chemicals will provide insights into how they may influence overall health and contribute to disease pathogenesis. Here, we have developed a high resolution accurate mass (HRAM) screening strategy allowing simultaneous identification and relative quantitation of DNPH-derivatized carbonyls in human biological fluids. The screening strategy involves the diagnostic neutral loss of hydroxyl radical triggering MS3 fragmentation, which is only observed in positive ionization mode of DNPH-derivatized carbonyls. Unique fragmentation pathways were used to develop a classification scheme for characterizing known and unanticipated/unknown carbonyl compounds present in saliva. Furthermore, a relative quantitation strategy was implemented to assess variations in the levels of carbonyl compounds before and after exposure using deuterated d3-DNPH. This relative quantitation method was tested on human samples before and after exposure to specific amounts of alcohol. The nano-electrospray ionization (nano-ESI) in positive mode afforded excellent sensitivity with detection limits on-column in the high-attomole levels. To the best of our knowledge, this is the first report of a method using HRAM neutral loss screening of carbonyl compounds. In addition, the method allows simultaneous characterization and relative quantitation of DNPH-derivatized compounds using nano-ESI in positive mode.
机译:反应性羰基化合物(RCC)在环境中无处不在,是由于各种生理和病理过程而内生产生的。这些化合物可与生物分子反应,诱导有害过程,认为这是其毒性作用的基础。这些化合物中的几种被认为与神经毒性过程,衰老疾病和癌症有关。因此,表征暴露于这些化学物质的方法将提供有关它们如何影响整体健康并促进疾病发病机理的见解。在这里,我们已经开发了一种高分辨率精确质量(HRAM)筛选策略,可以同时鉴定和定量定量DNPH衍生的人类生物流体中的羰基。筛选策略涉及诊断羟自由基引发MS 3 断裂的中性丢失,这仅在DNPH衍生的羰基的正电离模式下才能观察到。使用独特的片段化途径来开发分类方案,以表征唾液中已知和未预期/未知的羰基化合物。此外,实施了相对定量策略,以评估使用氘代d3-DNPH暴露前后羰基化合物含量的变化。在暴露于特定量的酒精之前和之后,在人体样品上测试了这种相对定量方法。处于正模式的纳米电喷雾电离(nano-ESI)提供了出色的灵敏度,并且在高原子水平上的柱上检测极限。据我们所知,这是使用HRAM对羰基化合物进行中性损失筛选的方法的首次报道。另外,该方法允许使用正模式的纳米ESI同时表征和相对定量DNPH衍生的化合物。

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