脂肪酸去饱和酶插入/缺失多态性 rs66698963 预测 n-3 脂肪酸二十碳五烯酸预防结直肠息肉:SEAFood 息肉预防试验的二次分析。
Fatty acid desaturase insertion-deletion polymorphism rs66698963 predicts colorectal polyp prevention by the n-3 fatty acid eicosapentaenoic acid: a secondary analysis of the seAFOod polyp prevention trial.
机构信息
Leeds Institute of Medical Research, University of Leeds, Leeds, United Kingdom.
Department of Pediatrics, Dell Pediatric Research Institute, Dell Medical School, The University of Texas at Austin, TX, United States; Department of Nutritional Sciences, The University of Texas at Austin, Austin, TX, United States.
出版信息
Am J Clin Nutr. 2024 Aug;120(2):360-368. doi: 10.1016/j.ajcnut.2024.06.004. Epub 2024 Jun 13.
BACKGROUND
A fatty acid desaturase (FADS) insertion-deletion (Indel) polymorphism (rs66698963) influences the expression of FADS1, which controls the synthesis of n-6 highly unsaturated fatty acid (HUFA) arachidonic acid (AA). The anti-inflammatory activity of the n-3 HUFA eicosapentaenoic acid (EPA) may be explained by competition with AA for proinflammatory lipid mediator synthesis. A precision medicine approach based on stratification by FADS Indel genotype could identify individuals, who benefit from greatest disease risk reduction by n-3 HUFAs.
OBJECTIVES
We tested the hypothesis that the FADS insertion (I) allele predicts colorectal polyp risk reduction in a secondary analysis of the randomized, placebo-controlled, 2×2 factorial seAFOod polyp prevention trial of EPA 2000 mg daily and aspirin 300 mg daily for 12 mo (ISRCTN05926847).
METHODS
Participant Indel genotype was determined by polymerase chain reaction (PCR) blind to trial outcomes. Colorectal polyp outcomes were included in negative binomial (polyp number) and logistic (polyp detection rate [PDR; percentage with one or more polyps]) regression models comparing each active intervention with its placebo. Presence of ≥1 Indel I allele and an interaction term (I allele × active intervention) were covariates.
RESULTS
In 528 participants with colonoscopy and FADS Indel data, EPA use irrespective of Indel genotype, was not associated with reduced colorectal polyp number (incidence rate ratio [IRR]: 0.92; 95% confidence interval: 0.74, 1.16), mirroring original seAFOod trial analysis. However, the presence of ≥1 I allele identified EPA users with a significant reduction in colorectal polyp number (IRR: 0.50 [0.28, 0.90]), unlike aspirin, for which there was no interaction. Similar findings were obtained for the PDR.
CONCLUSIONS
The FADS Indel I allele identified individuals, who displayed colorectal polyp prevention by EPA with a similar effect size to aspirin. Assessment of rs66698963 as a biomarker of therapeutic response to n-3 HUFAs in other populations and healthcare settings is warranted. The seAFOod polyp prevention trial and STOP-ADENOMA study were registered at International Standard Randomised Controlled Trial Number registry as ISRCTN05926847.
背景
脂肪酸去饱和酶(FADS)插入/缺失(Indel)多态性(rs66698963)影响 FADS1 的表达,而 FADS1 控制着 n-6 高度不饱和脂肪酸(HUFA)花生四烯酸(AA)的合成。n-3 HUFA 二十碳五烯酸(EPA)的抗炎活性可以通过与 AA 竞争促炎脂质介质的合成来解释。基于 FADS Indel 基因型分层的精准医学方法可以识别出通过 n-3 HUFAs 最大程度降低疾病风险的个体。
目的
我们通过对 EPA 2000mg/d 和阿司匹林 300mg/d 每日治疗 12 个月的随机、安慰剂对照、2×2 析因 seAFOod 息肉预防试验(ISRCTN05926847)的二次分析,检验 FADS 插入(I)等位基因预测结直肠息肉风险降低的假设。
方法
通过聚合酶链反应(PCR)盲法检测参与者的 Indel 基因型,而不考虑试验结果。结直肠息肉结局纳入负二项式(息肉数量)和逻辑(息肉检出率[PDR;有一个或多个息肉的百分比])回归模型,将每种活性干预与安慰剂进行比较。存在≥1 Indel I 等位基因和交互项(I 等位基因×活性干预)为协变量。
结果
在 528 名接受结肠镜检查和 FADS Indel 数据分析的参与者中,无论 Indel 基因型如何,EPA 的使用均与结直肠息肉数量的减少无关(发病率比[IRR]:0.92;95%置信区间:0.74,1.16),与原始 seAFOod 试验分析一致。然而,存在≥1 I 等位基因可识别 EPA 使用者的结直肠息肉数量显著减少(IRR:0.50[0.28,0.90]),而阿司匹林则没有交互作用。PDR 也有类似的发现。
结论
FADS Indel I 等位基因鉴定出了 EPA 可预防结直肠息肉的个体,其效果大小与阿司匹林相似。评估 rs66698963 作为其他人群和医疗保健环境中 n-3 HUFAs 治疗反应的生物标志物是合理的。seAFOod 息肉预防试验和 STOP-ADENOMA 研究在国际标准随机对照试验注册处注册为 ISRCTN05926847。
Zotero 插件