胎盘脂肪酸去饱和酶2 (FADS2)甲基化与子痫前期妇女母体脂肪酸水平的关系

IF 3 Prostaglandins, leukotrienes, and essential fatty acids Pub Date : 2022-09-01 DOI:10.1016/j.plefa.2022.102472

Kinjal Dave , Lovejeet Kaur , Deepali Sundrani , Preeti Sharma , Swati Bayyana , Savita Mehendale , Karuna Randhir , Giriraj R Chandak , Sadhana Joshi

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引用次数: 3

摘要

长链多不饱和脂肪酸的生物合成需要脂肪酸前体转化为产物的去饱和酶和延伸酶的顺序活性。由FADS2基因编码的δ -6去饱和酶是该途径中的限速酶。D6D酶活性的改变可导致脂肪酸谱的改变。目的探讨子痫前期妇女胎盘DNA甲基化(DNAm)和FADS2基因表达与正常妇女的差异及其与母体变量(血浆脂肪酸、去饱和酶指数、血压)、胎盘重量和分娩结局的关系。方法采用焦磷酸测序法和实时荧光定量PCR法分别检测正常血压组(n = 100)和子痫前期组(n = 100)胎盘中sdnam和FADS2基因的表达。先兆子痫妇女包括足月分娩的妇女(n = 43，妊娠≥37周;T-PE)或早产(n = 57，妊娠<37周;各)。结果1区13个CpGs中，T-PE中CpG3高甲基化显著(p = 0.03); 2区13个CpGs中，与对照组相比，CpG2 (p = 0.008)、CpG11 (p = 0.04)、CpG12 (p = 0.001)低甲基化，CpG13高甲基化(p = 0.001)。PT-PE中FADS2表达低于对照组(p = 0.04)。FADS2中不同CpGs的DNAm与母体血浆FADS2酶指数相关，也与母体脂肪酸水平相关。然而，我们没有观察到dna与产妇血压、胎盘重量和分娩结局有任何关联。本研究首次报道了FADS2甲基化差异及其与子痫前期母体脂肪酸代谢受损的关系，并为我们早期观察子痫前期女性母体LCPUFA水平改变提供了机制基础。

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Association of placental fatty acid desaturase 2 (FADS2) methylation with maternal fatty acid levels in women with preeclampsia

Introduction

Biosynthesis of long-chain polyunsaturated fatty acids requires sequential activities of desaturases and elongases for conversion of fatty acid precursors to products. The delta-6 desaturase enzyme, encoded by FADS2 gene, is a rate limiting enzyme in this pathway. Alterations in D6D enzyme activity can lead to altered fatty acid profiles.

Objectives

To examine differences in placental DNA methylation (DNAm) and expression of FADS2 gene in preeclampsia women compared to normal women and their association with maternal variables (plasma fatty acids, desaturase enzyme index, blood pressure), placental weight and birth outcomes.

Methods

DNAm and expression of FADS2 gene were examined in placentae of normotensive (n = 100) control and preeclampsia (n = 100) women using pyrosequencing and quantitative real-time PCR respectively. Women with preeclampsia included those delivering at term (n = 43, gestation ≥ 37 weeks; T-PE) or preterm (n = 57, gestation < 37 weeks; PT-PE). A total of 26 CpGs in FADS2 promoter and region around it, were analysed in two PCR reactions (region 1 and 2).

Results

Out of 13 CpGs in region 1, significant hypermethylation was noted at CpG3 in T-PE (p = 0.03) and of 13 CpGs in region 2, CpG2 (p = 0.008), CpG11 (p = 0.04), CpG12 (p = 0.001) were hypomethylated and CpG13 (p = 0.001) was hypermethylated in preeclampsia group, as compared to controls. FADS2 expression was lower in PT-PE as compared to controls (p = 0.04). DNAm at various CpGs in the FADS2 were associated with maternal plasma FADS2 enzyme index and also associated with maternal fatty acid levels. However, we did not observe any association of DNAm with maternal blood pressure, placental weight and birth outcomes.

Conclusions

This study for the first time reports differential methylation of FADS2 and its association with impaired maternal fatty acid metabolism in preeclampsia and provides a mechanistic basis to our earlier observations of altered maternal LCPUFA levels in women with preeclampsia.

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