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出生时的 DNA 甲基化模式可预测极低出生体重儿成年后的健康结果。

DNA methylation patterns at birth predict health outcomes in young adults born very low birthweight.

机构信息

Christchurch Heart Institute, Department of Medicine, University of Otago, Christchurch, PO Box 4345, Christchurch, 8140, New Zealand.

Department of Surgical Sciences, University of Otago, Dunedin, New Zealand.

出版信息

Clin Epigenetics. 2023 Mar 23;15(1):47. doi: 10.1186/s13148-023-01463-3.

Abstract

BACKGROUND

Individuals born very low birthweight (VLBW) are at increased risk of impaired cardiovascular and respiratory function in adulthood. To identify markers to predict future risk for VLBW individuals, we analyzed DNA methylation at birth and at 28 years in the New Zealand (NZ) VLBW cohort (all infants born < 1500 g in NZ in 1986) compared with age-matched, normal birthweight controls. Associations between neonatal methylation and cardiac structure and function (echocardiography), vascular function and respiratory outcomes at age 28 years were documented.

RESULTS

Genomic DNA from archived newborn heel-prick blood (n = 109 VLBW, 51 controls) and from peripheral blood at ~ 28 years (n = 215 VLBW, 96 controls) was analyzed on Illumina Infinium MethylationEPIC 850 K arrays. Following quality assurance and normalization, methylation levels were compared between VLBW cases and controls at both ages by linear regression, with genome-wide significance set to p < 0.05 adjusted for false discovery rate (FDR, Benjamini-Hochberg). In neonates, methylation at over 16,400 CpG methylation sites differed between VLBW cases and controls and the canonical pathway most enriched for these CpGs was Cardiac Hypertrophy Signaling (p = 3.44E). The top 20 CpGs that differed most between VLBW cases and controls featured clusters in ARID3A, SPATA33, and PLCH1 and these 3 genes, along with MCF2L, TRBJ2-1 and SRC, led the list of 15,000 differentially methylated regions (DMRs) reaching FDR-adj significance. Fifteen of the 20 top CpGs in the neonate EWAS showed associations between methylation at birth and adult cardiovascular traits (particularly LnRHI). In 28-year-old adults, twelve CpGs differed between VLBW cases and controls at FDR-adjusted significance, including hypermethylation in EBF4 (four CpGs), CFI and UNC119B and hypomethylation at three CpGs in HIF3A and one in KCNQ1. DNA methylation GrimAge scores at 28 years were significantly greater in VLBW cases versus controls and weakly associated with cardiovascular traits. Four CpGs were identified where methylation differed between VLBW cases and controls in both neonates and adults, three reversing directions with age (two CpGs in EBF4, one in SNAI1 were hypomethylated in neonates, hypermethylated in adults). Of these, cg16426670 in EBF4 at birth showed associations with several cardiovascular traits in adults.

CONCLUSIONS

These findings suggest that methylation patterns in VLBW neonates may be informative about future adult cardiovascular and respiratory outcomes and have value in guiding early preventative care to improve adult health.

摘要

背景

极低出生体重(VLBW)的个体在成年后心血管和呼吸系统功能受损的风险增加。为了确定预测 VLBW 个体未来风险的标志物,我们分析了新西兰 VLBW 队列(1986 年在新西兰出生体重<1500 克的所有婴儿)中新生儿和 28 岁时的 DNA 甲基化情况,并与年龄匹配的正常出生体重对照组进行了比较。记录了新生儿甲基化与 28 岁时的心脏结构和功能(超声心动图)、血管功能和呼吸结局之间的关联。

结果

对存档的新生儿足跟采血(n=109 例 VLBW,51 例对照)和外周血(n=215 例 VLBW,96 例对照)的基因组 DNA 进行了 Illumina Infinium MethylationEPIC 850K 芯片分析。在经过质量保证和归一化后,通过线性回归比较了 VLBW 病例和对照组在两个年龄组之间的甲基化水平,全基因组显著性设置为 p<0.05,调整了假发现率(FDR,Benjamini-Hochberg)。在新生儿中,VLBW 病例和对照组之间有超过 16400 个 CpG 甲基化位点的甲基化水平不同,这些 CpG 最富集的典型途径是心脏肥大信号通路(p=3.44E)。在 VLBW 病例和对照组之间差异最大的前 20 个 CpG 特征在于 ARID3A、SPATA33 和 PLCH1 中的簇,这些基因与 MCF2L、TRBJ2-1 和 SRC 一起,领衔 15000 个差异甲基化区域(DMRs)的名单,达到 FDR 调整显著性。新生儿 EWAS 中前 20 个 CpG 中有 15 个与成年心血管特征(尤其是 LnRHI)之间存在出生时的甲基化关联。在 28 岁的成年人中,12 个 CpG 在 FDR 调整显著性上存在 VLBW 病例和对照组之间的差异,包括 EBF4(四个 CpG)、CFI 和 UNC119B 的过度甲基化以及 HIF3A 中的三个 CpG 和 KCNQ1 中的一个 CpG 的低甲基化。28 岁时,VLBW 病例的 DNA 甲基化 GrimAge 评分明显高于对照组,并且与心血管特征呈弱相关。有四个 CpG 被确定为 VLBW 病例和对照组在新生儿和成年人中存在甲基化差异,其中三个 CpG 随着年龄的变化而变化(EBF4 中的两个 CpG,SNAI1 中的一个 CpG 在新生儿时呈低甲基化,在成年人时呈高甲基化)。其中,EBF4 中的 cg16426670 在出生时与成年人的几个心血管特征有关。

结论

这些发现表明,VLBW 新生儿的甲基化模式可能与未来的成年人心血管和呼吸结局有关,并对指导早期预防保健以改善成年健康具有重要价值。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c108/10035230/af2cd5de475d/13148_2023_1463_Fig1_HTML.jpg

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