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Epigenome-wide association study identifies DNA methylation markers for asthma remission in blood and nasal epithelium

Authors :
Cancan Qi
Gerard H. Koppelman
Diana A van der Plaat
Nicole Dijk
Judith M. Vonk
Valérie Siroux
Maartje A.E. Nieuwenhuis
Dylan Aïssi
Cheng-Jian Xu
Hendrika Boezen
Publication Year :
2020
Publisher :
Authorea, Inc., 2020.

Abstract

Background: Asthma is a chronic respiratory disease which is not curable, yet some patients experience spontaneous remission. We hypothesized that epigenetic mechanisms may be involved in asthma remission. Methods: Clinical remission (ClinR) was defined as the absence of asthma symptoms and medication for at least 12 months, and complete remission (ComR) was defined as ClinR with normal lung function and absence of airway hyperresponsiveness. We analyzed differential DNA methylation of ClinR and ComR comparing to persistent asthma (PersA) in whole blood samples (n=72) and nasal brushing samples (n=97) in a longitudinal cohort of well characterized asthma patients. Significant findings of whole blood DNA methylation were tested for replication in two independent cohorts, Lifelines and EGEA. Results: We identified differentially methylated CpG sites associated with ClinR (7 CpG sites) and ComR (129 CpG sites) in whole blood. One CpG (cg13378519, Chr1) associated with ClinR was replicated and annotated to PEX11 (Peroxisomal Biogenesis Factor 11 Beta). The whole blood DNA methylation levels of this CpG were also different between ClinR and healthy subjects. One ComR-associated CpG (cg24788483, Chr10) that annotated to TCF7L2 (Transcription Factor 7 Like 2) was replicated and associated with expression of TCF7L2 gene. One out of seven ClinR-associated CpG sites and 8 out of 129 ComR-associated CpG sites identified from whole blood samples showed nominal significance (P

Details

Database :
OpenAIRE
Accession number :
edsair.doi...........2ba977c0e20aa1cbffe998c06942456e