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妊娠期间糖代谢异常的代谢驱动因素:英国多民族出生队列中 146 种代谢物的种族特异性 GWAS 和 1 样本 Mendelian 随机化分析。

Metabolic drivers of dysglycemia in pregnancy: ethnic-specific GWAS of 146 metabolites and 1-sample Mendelian randomization analyses in a UK multi-ethnic birth cohort.

机构信息

School of Food Science and Nutrition, University of Leeds, Leeds, United Kingdom.

Public Health Science Division, Fred Hutchinson Cancer Center, Seattle, WA, United States.

出版信息

Front Endocrinol (Lausanne). 2023 May 15;14:1157416. doi: 10.3389/fendo.2023.1157416. eCollection 2023.

Abstract

INTRODUCTION

Gestational diabetes mellitus (GDM) is the most common pregnancy complication worldwide and is associated with short- and long-term health implications for both mother and child. Prevalence of GDM varies between ethnicities, with South Asians (SAs) experiencing up to three times the risk compared to white Europeans (WEs). Recent evidence suggests that underlying metabolic difference contribute to this disparity, but an investigation of causality is required.

METHODS

To address this, we paired metabolite and genomic data to evaluate the causal effect of 146 distinct metabolic characteristics on gestational dysglycemia in SAs and WEs. First, we performed 292 GWASs to identify ethnic-specific genetic variants associated with each metabolite (P ≤ 1 x 10-5) in the Born and Bradford cohort (3688 SA and 3354 WE women). Following this, a one-sample Mendelian Randomisation (MR) approach was applied for each metabolite against fasting glucose and 2-hr post glucose at 26-28 weeks gestation. Additional GWAS and MR on 22 composite measures of metabolite classes were also conducted.

RESULTS

This study identified 15 novel genome-wide significant (GWS) SNPs associated with tyrosine in the FOXN and SLC13A2 genes and 1 novel GWS SNP (currently in no known gene) associated with acetate in SAs. Using MR approach, 14 metabolites were found to be associated with postprandial glucose in WEs, while in SAs a distinct panel of 11 metabolites were identified. Interestingly, in WEs, cholesterols were the dominant metabolite class driving with dysglycemia, while in SAs saturated fatty acids and total fatty acids were most commonly associated with dysglycemia.

DISCUSSION

In summary, we confirm and demonstrate the presence of ethnic-specific causal relationships between metabolites and dysglycemia in mid-pregnancy in a UK population of SA and WE pregnant women. Future work will aim to investigate their biological mechanisms on dysglycemia and translating this work towards ethnically tailored GDM prevention strategies.

摘要

简介

妊娠糖尿病(GDM)是全球最常见的妊娠并发症,会对母婴的短期和长期健康产生影响。GDM 的患病率在不同种族之间存在差异,南亚人(SAs)的患病风险比白种欧洲人(WEs)高 3 倍。最近的证据表明,潜在的代谢差异导致了这种差异,但需要进行因果关系的调查。

方法

为了解决这个问题,我们将代谢物和基因组数据配对,以评估 146 种不同的代谢特征对南亚人和白种欧洲人妊娠性血糖紊乱的因果影响。首先,我们在出生和布拉德福德队列中进行了 292 项全基因组关联研究(GWAS),以确定与每种代谢物相关的特定种族的遗传变异(P ≤ 1 x 10-5)(3688 名南亚人和 3354 名白种欧洲人女性)。在此之后,我们对每个代谢物进行了单样本孟德尔随机化(MR)分析,以对抗 26-28 周妊娠时的空腹血糖和 2 小时餐后血糖。还对 22 种代谢物类别的综合测量进行了额外的 GWAS 和 MR 分析。

结果

这项研究在 FOXN 和 SLC13A2 基因中发现了与酪氨酸相关的 15 个新的全基因组显著(GWS)SNP,在南亚人中发现了与乙酸盐相关的 1 个新的全基因组显著(GWS)SNP(目前尚未发现已知基因)。使用 MR 方法,在 WEs 中发现 14 种代谢物与餐后血糖相关,而在 SAs 中则发现了一组不同的 11 种代谢物。有趣的是,在 WEs 中,胆固醇是导致血糖紊乱的主要代谢物类别,而在 SAs 中,饱和脂肪酸和总脂肪酸与血糖紊乱最常见相关。

讨论

总之,我们在英国的南亚和白种欧洲孕妇人群中证实并证明了妊娠中期代谢物与血糖紊乱之间存在特定种族的因果关系。未来的工作将旨在研究它们对血糖紊乱的生物学机制,并将这项工作转化为针对特定种族的 GDM 预防策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7ece/10225646/5524679f56b1/fendo-14-1157416-g001.jpg

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