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通过毛细管液相色谱结合双在线光电二极管阵列和串联质谱检测进行综合分析,对缺氧肺组织进行直接类二十烷酸谱分析。

Direct eicosanoid profiling of the hypoxic lung by comprehensive analysis via capillary liquid chromatography with dual online photodiode-array and tandem mass-spectrometric detection.

作者信息

Kiss Ladislau, Röder Yasmin, Bier Jens, Weissmann Norbert, Seeger Werner, Grimminger Friedrich

机构信息

Biochemie Med. II, University of Giessen Lung Center, Department of Internal Medicine, Justus Liebig University, Paul Meimberg Str. 5, 35392, Giessen, Germany.

出版信息

Anal Bioanal Chem. 2008 Jan;390(2):697-714. doi: 10.1007/s00216-007-1718-9. Epub 2007 Dec 14.

Abstract

Eicosanoids are arachidonic acid-derived mediators, with partly contradictory, incompletely elucidated actions. Thus, epoxyeicosatrienoic acids (EETs) are controversially discussed as putative vasodilatative endothelium-derived hyperpolarizing factors in the cardiovascular compartment but reported as vasoconstrictors in the lung. Inconsistent findings concerning eicosanoid physiology may be because previous methods were lacking sensitivity, identification reliability, and/or have focused on special eicosanoid groups only, ignoring the overall mediator context, and thus limiting the correlation accuracy between autacoid formation and bioactivity profile. Therefore, we developed an approach which enables the simultaneous assessment of 44 eicosanoids, including all representatives of the arachidonic acid cascade, i.e., cytochrome P450, lipoxygenase, cyclooxygenase products, and free isoprostanes as in vivo markers of oxidative stress, in one 50-minute chromatographic run. The approach combines (i) source-specific sample extraction, (ii) rugged isocratic and high-sensitivity capillary liquid-chromatographic separation, and (iii) reliable dual online photodiode-array and electrospray ionization tandem mass-spectrometric identification and quantitation. High sensitivity with limits of quantification in the femtogram range was achieved by use of capillary columns with typical high peak efficiency, due to small inner diameters, and virtually complete substance transfer to the mass spectrometer, due to flow rates in the low microliter range, instead of large inner diameter columns with low chromatographic signal and only partial analyte transfer employed by previous methods. This expeditious, global and sensitive technique provides the prerequisite for new, accurate insights regarding the physiology of specific mediators, for example EETs, in the context of all relevant vasoactive autacoids under varying conditions of oxidative stress by direct comparison of all eicosanoid generation profiles. Indeed, application of comprehensive "eicoprofiling" to hypoxically ventilated rabbit lungs revealed at a glance the enhanced biosynthesis of free EETs in the overall mediator generation context, thus suggesting their hypothetical contribution to hypoxic pulmonary vasoconstriction.

摘要

类二十烷酸是花生四烯酸衍生的介质,其作用部分相互矛盾,尚未完全阐明。因此,环氧二十碳三烯酸(EETs)作为心血管系统中假定的血管舒张性内皮衍生超极化因子存在争议,但在肺中被报道为血管收缩剂。关于类二十烷酸生理学的不一致发现可能是因为先前的方法缺乏敏感性、鉴定可靠性,和/或仅关注特殊的类二十烷酸组,忽略了整体介质环境,从而限制了自分泌物质形成与生物活性谱之间的相关性准确性。因此,我们开发了一种方法,能够在一次50分钟的色谱运行中同时评估44种类二十烷酸,包括花生四烯酸级联反应的所有代表物,即细胞色素P450、脂氧合酶、环氧化酶产物,以及作为氧化应激体内标志物的游离异前列腺素。该方法结合了(i)源特异性样品提取,(ii)耐用的等度和高灵敏度毛细管液相色谱分离,以及(iii)可靠的双在线光电二极管阵列和电喷雾电离串联质谱鉴定与定量。通过使用具有典型高柱效的毛细管柱实现了飞克级范围内的高灵敏度定量限,这是由于内径小,以及由于低微升范围内的流速,几乎完全将物质转移到质谱仪中,而不是先前方法中使用的具有低色谱信号且仅部分分析物转移的大内径柱。这种快速、全面且灵敏的技术为在氧化应激不同条件下,通过直接比较所有类二十烷酸生成谱,在所有相关血管活性自分泌物质的背景下,对特定介质(例如EETs)的生理学进行新的、准确的深入研究提供了前提条件。事实上,将全面的“类二十烷酸谱分析”应用于低氧通气的兔肺,一眼就揭示了在整体介质生成背景下游离EETs生物合成的增强,从而表明它们对低氧性肺血管收缩的假设贡献。

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