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Stereoselective oxidation of regioisomeric octadecenoic acids by fatty acid dioxygenases

机译:脂肪酸双加氧酶对立体异构十八碳烯酸的立体选择性氧化

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摘要

Seven Z-octadecenoic acids having the double bond located in positions 6Z to 13Z were photooxidized. The resulting hydroperoxy-E-octadecenoic acids [HpOME(E)] were resolved by chiral phase-HPLC-MS, and the absolute configurations of the enantiomers were determined by gas chromatographic analysis of diastereoisomeric derivatives. The MS/MS/MS spectra showed characteristic fragments, which were influenced by the distance between the hydroperoxide and carboxyl groups. These fatty acids were then investigated as substrates of cyclooxygenase-1 (COX-1), manganese lipoxygenase (MnLOX), and the (8R)-dioxygenase (8R-DOX) activities of two linoleate diol synthases (LDS) and 10R-DOX. COX-1 and MnLOX abstracted hydrogen at C-11 of (12Z)-18:1 and C-12 of (13Z)-18:1. (11Z)-18:1 was subject to hydrogen abstraction at C-10 by MnLOX and at both allylic positions by COX-1. Both allylic hydrogens of (8Z)-18:1 were also abstracted by 8R-DOX activities of LDS and 10R-DOX, but only the allylic hydrogens close to the carboxyl groups of (11Z)-18:1 and (12Z)-18:1. 8R-DOX also oxidized monoenoic C14-C20 fatty acids with double bonds at the (9Z) position, suggesting that the length of the omega end has little influence on positioning for oxygenation. We conclude that COX-1 and MnLOX can readily abstract allylic hydrogens of octadecenoic fatty acids from C-10 to C-12 and 8R-DOX from C-7 and C-12.
机译:将位于6Z至13Z位置的具有双键的七个Z-十八烯酸光氧化。通过手性相-HPLC-MS拆分得到的氢过氧-E-十八烯酸[HpOME(E)],并通过非对映异构体衍生物的气相色谱分析确定对映异构体的绝对构型。 MS / MS / MS谱图显示了特征性片段,这些片段受氢过氧化物和羧基之间的距离影响。然后研究这些脂肪酸作为环氧化酶-1(COX-1),锰脂氧化酶(MnLOX)和两种亚油酸二醇合酶(LDS)和10R-DOX的(8R)-双加氧酶(8R-DOX)活性的底物。 COX-1和MnLOX在(12Z)-18:1的C-11和(13Z)-18:1的C-12处提取氢。 (11Z)-18:1在Mn-10处在C-10处被夺氢,在COX-1上的两个烯丙基位置处被夺氢。 LDS和10R-DOX的8R-DOX活性也提取了(8Z)-18:1的两个烯丙基氢,但只有接近(11 Z - 18:1和(12 Z - 18:1。 8 R -DOX还氧化了在(9 Z )位置具有双键的单烯键式C14-C20脂肪酸,这表明欧米茄末端的长度对位置的影响很小充氧。我们得出结论,COX-1和MnLOX可以很容易地从C-10到C-12提取十八烯脂肪酸的烯丙基氢,并从C-7和C-12提取8 R -DOX。

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