Leeds Institute of Medical Research, University of Leeds, UK.
Institute of Cancer Therapeutics, University of Bradford, UK.
Prostaglandins Leukot Essent Fatty Acids. 2023 May;192:102570. doi: 10.1016/j.plefa.2023.102570. Epub 2023 Mar 23.
Aspirin and eicosapentaenoic acid (EPA) have colorectal polyp prevention activity, alone and in combination. This study measured levels of plasma and rectal mucosal oxylipins in participants of the seAFOod 2 × 2 factorial, randomised, placebo-controlled trial, who received aspirin 300 mg daily and EPA 2000 mg free fatty acid, alone and in combination, for 12 months.
Resolvin (Rv) E1, 15-epi-lipoxin (LX) A and respective precursors 18-HEPE and 15-HETE (with chiral separation) were measured by ultra-high performance liquid chromatography-tandem mass spectrometry in plasma taken at baseline, 6 months and 12 months, as well as rectal mucosa obtained at trial exit colonoscopy at 12 months, in 401 trial participants.
Despite detection of S- and R- enantiomers of 18-HEPE and 15-HETE in ng/ml concentrations, RvE1 or 15‑epi-LXA were not detected above a limit of detection of 20 pg/ml in plasma or rectal mucosa, even in individuals randomised to both aspirin and EPA. We have confirmed in a large clinical trial cohort that prolonged (12 months) treatment with EPA is associated with increased plasma 18-HEPE concentrations (median [inter-quartile range] total 18-HEPE 0.51 [0.21-1.95] ng/ml at baseline versus 0.95 [0.46-4.06] ng/ml at 6 months [P<0.0001] in those randomised to EPA alone), which correlate strongly with respective rectal mucosal 18-HEPE levels (r = 0.82; P<0.001), but which do not predict polyp prevention efficacy by EPA or aspirin.
Analysis of seAFOod trial plasma and rectal mucosal samples has not provided evidence of synthesis of the EPA-derived specialised pro-resolving mediator RvE1 or aspirin-trigged lipoxin 15‑epi-LXA. We cannot rule out degradation of individual oxylipins during sample collection and storage but readily measurable precursor oxylipins argues against widespread degradation.
阿司匹林和二十碳五烯酸(EPA)单独或联合使用均具有预防结肠息肉的作用。本研究测量了接受每日 300mg 阿司匹林和 2000mg 游离脂肪酸 EPA 单独及联合治疗 12 个月的 seAFOod 2×2 析因、随机、安慰剂对照试验参与者的血浆和直肠黏膜氧化脂水平。
采用超高效液相色谱-串联质谱法测定基线、6 个月和 12 个月时的血浆中 RvE1、15-epi-LXA 和各自的前体 18-HEPE 和 15-HETE(采用手性分离),以及 12 个月时试验结束结肠镜检查时的直肠黏膜,共纳入 401 名试验参与者。
尽管以 ng/ml 浓度检测到 S-和 R-对映体 18-HEPE 和 15-HETE,但在血浆或直肠黏膜中均未检测到 RvE1 或 15-epi-LXA 的检测限以上,即使在随机分配到阿司匹林和 EPA 的个体中也是如此。我们在一个大型临床试验队列中证实,延长(12 个月)EPA 治疗与血浆 18-HEPE 浓度升高相关(基线时总 18-HEPE 的中位数[四分位距]为 0.51[0.21-1.95]ng/ml,而单独接受 EPA 治疗的患者在 6 个月时为 0.95[0.46-4.06]ng/ml[P<0.0001]),这与相应的直肠黏膜 18-HEPE 水平密切相关(r=0.82;P<0.001),但不能预测 EPA 或阿司匹林的息肉预防疗效。
对 seAFOod 试验血浆和直肠黏膜样本的分析并未提供 EPA 衍生的特殊促解决介质 RvE1 或阿司匹林触发的脂氧素 15-epi-LXA 合成的证据。我们不能排除在样本采集和储存过程中个别氧化脂的降解,但可轻易测量的前体氧化脂则表明广泛降解的可能性不大。
