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体外和体内二十二碳六烯酸过氧化生成神经前列腺素的区域化学。

Regiochemistry of neuroprostanes generated from the peroxidation of docosahexaenoic acid in vitro and in vivo.

作者信息

Yin Huiyong, Musiek Erik S, Gao Ling, Porter Ned A, Morrow Jason D

机构信息

Department of Pharmacology, Division of Clinical Pharmacology, Center in Molecular Toxicology and Vanderbilt Institute of Chemical Biology, Vanderbilt University, Nashville, Tennessee 37235, USA.

出版信息

J Biol Chem. 2005 Jul 15;280(28):26600-11. doi: 10.1074/jbc.M503088200. Epub 2005 May 13.

Abstract

Isoprostanes (IsoPs) are isomers of prostaglandins that are generated from the free radical-initiated peroxidation of arachidonic acid (C20.4 omega-6). IsoPs exert potent bioactivity and are regarded as the "gold standard" to assess oxidative stress in various human diseases. Analogously, autoxidation of docosahexaenoic acid (DHA, C22.6 omega-3) generates an array of IsoP-like compounds that are termed neuroprostanes (NPs). A major class of NPs identified in vitro and in vivo contains F-type prostane rings and are know as F4-NPs. A number of different F4-NP regioisomers are formed from the peroxidation of DHA. Among the eight possible regioisomeric groups, we hypothesize that 4- and 20-series NPs are generated in greater amounts than other classes because the precursors that lead to regioisomers other than those of the 4- and 20-series can be further oxidized to form novel dioxolane-IsoP-like compounds, analogous to those generated from arachidonate. Various mass spectrometric approaches, including electron capture atmospheric pressure chemical ionization mass spectrometry, were utilized to analyze NPs formed in vitro and in vivo based on their characteristic fragmentation in the gas phase. Experimental results were consistent with our hypothesis that 4- and 20-series NP regioisomers are preferentially generated. The discovery of regioselectivity in the formation of NPs will allow studies of the biological activities of NPs to focus on the more abundantly generated compounds to determine their role in modulating the pathophysiological consequences of DHA oxidation and oxidant stress.

摘要

异前列腺素(IsoPs)是前列腺素的异构体,由自由基引发的花生四烯酸(C20:4 ω-6)过氧化反应生成。异前列腺素具有强大的生物活性,被视为评估各种人类疾病中氧化应激的“金标准”。类似地,二十二碳六烯酸(DHA,C22:6 ω-3)的自氧化会产生一系列类似异前列腺素的化合物,被称为神经前列腺素(NPs)。在体外和体内鉴定出的一类主要的神经前列腺素含有F型前列腺环,被称为F4-神经前列腺素。许多不同的F4-神经前列腺素区域异构体由DHA的过氧化反应形成。在八个可能的区域异构体组中,我们推测4-和20-系列神经前列腺素的生成量比其他类别更多,因为导致4-和20-系列以外区域异构体的前体可以进一步氧化形成新型二氧戊环-异前列腺素样化合物,类似于由花生四烯酸生成的化合物。利用包括电子捕获大气压化学电离质谱在内的各种质谱方法,根据其在气相中的特征碎片来分析体外和体内形成的神经前列腺素。实验结果与我们的假设一致,即优先生成4-和20-系列神经前列腺素区域异构体。神经前列腺素形成过程中区域选择性的发现将使神经前列腺素生物活性的研究能够聚焦于生成量更多的化合物,以确定它们在调节DHA氧化和氧化应激的病理生理后果中的作用。

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