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Association of DOCK8, IL17RA, and KLK12 Polymorphisms with Atopic Dermatitis in Koreansopen access

Authors
Heo, Won IlPark, Kui YoungLee, Mi-KyungBae, Yu JeongMoon, Nam JuSeo, Seong Jun
Issue Date
Jun-2020
Publisher
KOREAN DERMATOLOGICAL ASSOC
Keywords
Atopic dermatitis; DOCK8; Exome sequencing; IL17RA; KLK12; Sanger sequencing
Citation
ANNALS OF DERMATOLOGY, v.32, no.3, pp 197 - 205
Pages
9
Journal Title
ANNALS OF DERMATOLOGY
Volume
32
Number
3
Start Page
197
End Page
205
URI
https://scholarworks.bwise.kr/cau/handle/2019.sw.cau/42574
DOI
10.5021/ad.2020.32.3.197
ISSN
1013-9087
2005-3894
Abstract
Background: Early-onset and severe atopic dermatitis (AD) in patients increase the probability of the development of allergic rhinitis or asthma. Treatment and prevention strategies in infants and young children with AD are targeted toward treating the symptoms, restoring skin barrier functions, and reducing the absorption of environmental allergens in an attempt to attenuate or block the onset of asthma and food allergy. Objective: Given that the initiating events in AD remain poorly understood, identifying those at risk and implementing strategies to prevent AD is necessary. Methods: Whole-exome sequencing (WES) was performed in a 43 control group and a disease group with 20 AD patients without atopic march (AM) and 20 with AM. Sanger sequencing was carried out to validate found variants in cohorts. Results: DOCK8, IL17RA, and KLK1 2 single-nucleotide polymorphisms were identified by WES as missense mutations: c.1289C> A, p.P97T (rs529208); c.1685C> A, p.P562G (rs12484684); and c.457+ 27>C, rs3745540, respectively. A case-control study show that total immunoglobulin E (IgE) level was significantly increased in the AA genotype of DOCK8 compared to the CA genotype in allergic patients. The rs12484684 of IL17RA increased risk of adult-onset AD (odds ratio: 1.63) compared to the control for (A) allele frequency. AD and AM Patients with the IL17RA CA genotype also had elevated IgE levels. rs3745540 of KLK12 was associated with AD in dominant model (odds ratio: 2.86). Conclusion: DOCK8 (rs529208), IL17RA (rs12484684), and KLK12 (rs3745540), were identified using a new WES filtering method. the result suggests that polymorphism of DOCK8 and IL17RA might be related to increase the total IgE level.
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