High-resolution Targeted Bisulfite Sequencing Reveals Blood Cell Type-specific DNA Methylation Patterns in IL13 and ORMDL3

Overview

Journal Clin Epigenetics

Publisher Biomed Central

Specialty Genetics

Date 2021 May 11

PMID 33971943

Citations 1

Authors

Cilla Soderhall

Lovisa E Reinius

Pertteli Salmenpera

Massimiliano Gentile

Nathalie Acevedo

Jon R Konradsen

Bjorn Nordlund

Gunilla Hedlin

Annika Scheynius

Samuel Myllykangas

Juha Kere

Affiliations

Soon will be listed here.

Abstract

Background: Methylation of DNA at CpG sites is an epigenetic modification and a potential modifier of disease risk, possibly mediating environmental effects. Currently, DNA methylation is commonly assessed using specific microarrays that sample methylation at a few % of all methylated sites.

Methods: To understand if significant information on methylation can be added by a more comprehensive analysis of methylation, we set up a quantitative method, bisulfite oligonucleotide-selective sequencing (Bs-OS-seq), and compared the data with microarray-derived methylation data. We assessed methylation at two asthma-associated genes, IL13 and ORMDL3, in blood samples collected from children with and without asthma and fractionated white blood cell types from healthy adult controls.

Results: Our results show that Bs-OS-seq can uncover vast amounts of methylation variation not detected by commonly used array methods. We found that high-density methylation information from even one gene can delineate the main white blood cell lineages.

Conclusions: We conclude that high-resolution methylation studies can yield clinically important information at selected specific loci missed by array-based methods, with potential implications for future studies of methylation-disease associations.

Citing Articles

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