Blood-Based EWAS of Asthma Polygenic Burden in The Netherlands Twin Register.

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Tác giả: Jeffrey J Beck, Dorret I Boomsma, Eco de Geus, Erik A Ehli, Casey T Finnicum, Jouke-Jan Hottenga, Patricia Huizenga, Brandon N Johnson, Noah Kallsen, René Pool, Austin J Van Asselt, Jenny van Dongen, Sarah Viet

Ngôn ngữ: eng

Ký hiệu phân loại: 949.2 *Netherlands

Thông tin xuất bản: Switzerland : Biomolecules , 2025

Mô tả vật lý:

Bộ sưu tập: NCBI

ID: 680725

 Asthma, a chronic respiratory condition characterized by airway inflammation, affects millions of individuals worldwide. Challenges remain in asthma prediction and diagnosis from its complex etiology involving genetic and environmental factors. Here, we investigated the relationship between genome-wide DNA methylation and genetic risk for asthma quantified via polygenic scores in two cohorts from the Netherlands Twin Register
  one enriched with asthmatic families measured on the Illumina EPIC array (n = 526) and a general population cohort measured on the Illumina HM450K array (n = 2680). We performed epigenome-wide association studies of asthma polygenic scores in each cohort with results combined through meta-analysis (total samples = 3206). The EWAS meta-analysis identified 63 significantly associated CpGs, (following Bonferroni correction, α = 0.05/358,316). An investigation of previous mQTL associations identified 48 mQTL associations between 24 unique CpGs and 48 SNPs, of which two SNPs have previous associations with asthma. Enrichment analysis using the 63 significant CpGs highlighted previous associations with ancestry, smoking, and air pollution. A dizygotic twin within-pair analysis of the 63 CpGs revealed similar directional effects between the two cohorts in 33 of the 63 CpGs. These findings further characterize the intricate relationship between DNA methylation and genetics relative to asthma.
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