Institut des Biomolécules Max Mousseron (IBMM,UMR5247 CNRS-UM1-UM2-ENSCM), Faculté de Pharmacie, 15 av. C. Flahault, BP.14491, 34093 Montpellier Cedex 5, France.
INSERM UMR 1060 (CarMeN), Université de Lyon, INSA-Lyon, Bldg Louis Pasteur, IMBL, 20 Av. A. Einstein, 69621 Villeurbanne, France.
Biochimie. 2014 Apr;99:1-7. doi: 10.1016/j.biochi.2013.11.006. Epub 2013 Nov 18.
There is currently a growing interest in docosahexaenoic acid (DHA) oxygenated metabolites. Among them, protectin D1 (PD1), an endogenous dihydroxylated and non-cyclic docosatriene made through lipoxygenation and hydrolysis of an epoxide intermediate, shows appealing biological effects. However, with the present paper we wish to point out that results are sometimes assigned to PD1 while they are indeed related to its isomer protectin DX (PDX) made through double lipoxygenation only. These misleading conclusions urge us to review herein the structural/chemical and biological differences in the docosatrienes reported to date in the literature i.e. PD1, the related PD1n-3 DPA, AT-NPD1, maresin 1 (MaR1) and MaR1n-3 DPA, as well as their poxytrin analogs such as PDX, and some synthetic diastereoisomers. Hopefully, this will avoid further mistakes and confusion in the future.
目前,人们对二十二碳六烯酸(DHA)的含氧代谢物越来越感兴趣。其中,保护素 D1(PD1)是一种内源性二羟基非环二十二碳三烯,通过环氧化物中间物的氧化和水解生成,具有吸引人的生物学效应。然而,本文旨在指出,有时将结果归因于 PD1,而实际上这些结果与它的异构体保护素 DX(PDX)有关,PDX 是通过双氧化作用仅生成的。这些误导性的结论促使我们回顾迄今为止文献中报道的二十二碳三烯的结构/化学和生物学差异,即 PD1、相关的 PD1n-3 DPA、AT-NPD1、maresin 1(MaR1)和 MaR1n-3 DPA 以及它们的环氧三烯类似物,如 PDX 和一些合成的非对映异构体。希望这将避免未来进一步的错误和混淆。
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