Replicated methylation changes associated with eczema herpeticum and allergic response

Meher Preethi Boorgula; Margaret A. Taub; Nicholas Rafaels; Michelle Daya; Monica Campbell; Sameer Chavan; Aniket Shetty; Chris Cheadle; Sangjucta Barkataki; Jinshui Fan; Gloria David; Terri H. Beaty; Ingo Ruczinski; Jon Hanifin; Lynda C. Schneider; Richard L. Gallo; Amy S. Paller; Lisa A. Beck; Donald Y. Leung; Rasika A. Mathias; Kathleen C. Barnes

doi:10.1186/s13148-019-0714-1

Replicated methylation changes associated with eczema herpeticum and allergic response

Meher Preethi Boorgula, Margaret A. Taub, Nicholas Rafaels, Michelle Daya, Monica Campbell, Sameer Chavan, Aniket Shetty, Chris Cheadle, Sangjucta Barkataki, Jinshui Fan, Gloria David, Terri H. Beaty, Ingo Ruczinski, Jon Hanifin, Lynda C. Schneider, Richard L. Gallo, Amy S. Paller, Lisa A. Beck, Donald Y. Leung, Rasika A. MathiasKathleen C. Barnes

Research output: Contribution to journal › Article › peer-review

6 Scopus citations

Abstract

Background: Although epigenetic mechanisms are important risk factors for allergic disease, few studies have evaluated DNA methylation differences associated with atopic dermatitis (AD), and none has focused on AD with eczema herpeticum (ADEH+). We will determine how methylation varies in AD individuals with/without EH and associated traits. We modeled differences in genome-wide DNA methylation in whole blood cells from 90 ADEH+, 83 ADEH-, and 84 non-atopic, healthy control subjects, replicating in 36 ADEH+, 53 ADEH-, and 55 non-atopic healthy control subjects. We adjusted for cell-type composition in our models and used genome-wide and candidate-gene approaches. Results: We replicated one CpG which was significantly differentially methylated by severity, with suggestive replication at four others showing differential methylation by phenotype or severity. Not adjusting for eosinophil content, we identified 490 significantly differentially methylated CpGs (ADEH+ vs healthy controls, genome-wide). Many of these associated with severity measures, especially eosinophil count (431/490 sites). Conclusions: We identified a CpG in IL4 associated with serum tIgE levels, supporting a role for Th2 immune mediating mechanisms in AD. Changes in eosinophil level, a measure of disease severity, are associated with methylation changes, providing a potential mechanism for phenotypic changes in immune response-related traits.

Original language	English (US)
Article number	122
Journal	Clinical Epigenetics
Volume	11
Issue number	1
DOIs	https://doi.org/10.1186/s13148-019-0714-1
State	Published - Aug 23 2019

Keywords

Atopic dermatitis
DNA methylation
Eczema herpeticum
Human epigenetics
Infinium Methylation 450K array
Methylation EPIC array

ASJC Scopus subject areas

Molecular Biology
Genetics
Developmental Biology
Genetics(clinical)

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10.1186/s13148-019-0714-1

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Boorgula, M. P., Taub, M. A., Rafaels, N., Daya, M., Campbell, M., Chavan, S., Shetty, A., Cheadle, C., Barkataki, S., Fan, J., David, G., Beaty, T. H., Ruczinski, I., Hanifin, J., Schneider, L. C., Gallo, R. L., Paller, A. S., Beck, L. A., Leung, D. Y., ... Barnes, K. C. (2019). Replicated methylation changes associated with eczema herpeticum and allergic response. Clinical Epigenetics, 11(1), Article 122. https://doi.org/10.1186/s13148-019-0714-1

Boorgula, MP, Taub, MA, Rafaels, N, Daya, M, Campbell, M, Chavan, S, Shetty, A, Cheadle, C, Barkataki, S, Fan, J, David, G, Beaty, TH , Ruczinski, I, Hanifin, J, Schneider, LC, Gallo, RL, Paller, AS, Beck, LA, Leung, DY, Mathias, RA & Barnes, KC 2019, 'Replicated methylation changes associated with eczema herpeticum and allergic response', Clinical Epigenetics, vol. 11, no. 1, 122. https://doi.org/10.1186/s13148-019-0714-1

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title = "Replicated methylation changes associated with eczema herpeticum and allergic response",

abstract = "Background: Although epigenetic mechanisms are important risk factors for allergic disease, few studies have evaluated DNA methylation differences associated with atopic dermatitis (AD), and none has focused on AD with eczema herpeticum (ADEH+). We will determine how methylation varies in AD individuals with/without EH and associated traits. We modeled differences in genome-wide DNA methylation in whole blood cells from 90 ADEH+, 83 ADEH-, and 84 non-atopic, healthy control subjects, replicating in 36 ADEH+, 53 ADEH-, and 55 non-atopic healthy control subjects. We adjusted for cell-type composition in our models and used genome-wide and candidate-gene approaches. Results: We replicated one CpG which was significantly differentially methylated by severity, with suggestive replication at four others showing differential methylation by phenotype or severity. Not adjusting for eosinophil content, we identified 490 significantly differentially methylated CpGs (ADEH+ vs healthy controls, genome-wide). Many of these associated with severity measures, especially eosinophil count (431/490 sites). Conclusions: We identified a CpG in IL4 associated with serum tIgE levels, supporting a role for Th2 immune mediating mechanisms in AD. Changes in eosinophil level, a measure of disease severity, are associated with methylation changes, providing a potential mechanism for phenotypic changes in immune response-related traits.",

keywords = "Atopic dermatitis, DNA methylation, Eczema herpeticum, Human epigenetics, Infinium Methylation 450K array, Methylation EPIC array",

author = "Boorgula, {Meher Preethi} and Taub, {Margaret A.} and Nicholas Rafaels and Michelle Daya and Monica Campbell and Sameer Chavan and Aniket Shetty and Chris Cheadle and Sangjucta Barkataki and Jinshui Fan and Gloria David and Beaty, {Terri H.} and Ingo Ruczinski and Jon Hanifin and Schneider, {Lynda C.} and Gallo, {Richard L.} and Paller, {Amy S.} and Beck, {Lisa A.} and Leung, {Donald Y.} and Mathias, {Rasika A.} and Barnes, {Kathleen C.}",

note = "Funding Information: Funding for this work was provided by NIH/NIAID U19 AI117673, The Atopic Dermatitis Research Network. KCB was supported in part by the Mary Beryl Patch Turnbull Scholar Program. Publisher Copyright: {\textcopyright} 2019 The Author(s).",

year = "2019",

month = aug,

day = "23",

doi = "10.1186/s13148-019-0714-1",

language = "English (US)",

volume = "11",

journal = "Clinical Epigenetics",

issn = "1868-7075",

publisher = "Springer Verlag",

number = "1",

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TY - JOUR

T1 - Replicated methylation changes associated with eczema herpeticum and allergic response

AU - Boorgula, Meher Preethi

AU - Taub, Margaret A.

AU - Rafaels, Nicholas

AU - Daya, Michelle

AU - Campbell, Monica

AU - Chavan, Sameer

AU - Shetty, Aniket

AU - Cheadle, Chris

AU - Barkataki, Sangjucta

AU - Fan, Jinshui

AU - David, Gloria

AU - Beaty, Terri H.

AU - Ruczinski, Ingo

AU - Hanifin, Jon

AU - Schneider, Lynda C.

AU - Gallo, Richard L.

AU - Paller, Amy S.

AU - Beck, Lisa A.

AU - Leung, Donald Y.

AU - Mathias, Rasika A.

AU - Barnes, Kathleen C.

N1 - Funding Information: Funding for this work was provided by NIH/NIAID U19 AI117673, The Atopic Dermatitis Research Network. KCB was supported in part by the Mary Beryl Patch Turnbull Scholar Program. Publisher Copyright: © 2019 The Author(s).

PY - 2019/8/23

Y1 - 2019/8/23

N2 - Background: Although epigenetic mechanisms are important risk factors for allergic disease, few studies have evaluated DNA methylation differences associated with atopic dermatitis (AD), and none has focused on AD with eczema herpeticum (ADEH+). We will determine how methylation varies in AD individuals with/without EH and associated traits. We modeled differences in genome-wide DNA methylation in whole blood cells from 90 ADEH+, 83 ADEH-, and 84 non-atopic, healthy control subjects, replicating in 36 ADEH+, 53 ADEH-, and 55 non-atopic healthy control subjects. We adjusted for cell-type composition in our models and used genome-wide and candidate-gene approaches. Results: We replicated one CpG which was significantly differentially methylated by severity, with suggestive replication at four others showing differential methylation by phenotype or severity. Not adjusting for eosinophil content, we identified 490 significantly differentially methylated CpGs (ADEH+ vs healthy controls, genome-wide). Many of these associated with severity measures, especially eosinophil count (431/490 sites). Conclusions: We identified a CpG in IL4 associated with serum tIgE levels, supporting a role for Th2 immune mediating mechanisms in AD. Changes in eosinophil level, a measure of disease severity, are associated with methylation changes, providing a potential mechanism for phenotypic changes in immune response-related traits.

AB - Background: Although epigenetic mechanisms are important risk factors for allergic disease, few studies have evaluated DNA methylation differences associated with atopic dermatitis (AD), and none has focused on AD with eczema herpeticum (ADEH+). We will determine how methylation varies in AD individuals with/without EH and associated traits. We modeled differences in genome-wide DNA methylation in whole blood cells from 90 ADEH+, 83 ADEH-, and 84 non-atopic, healthy control subjects, replicating in 36 ADEH+, 53 ADEH-, and 55 non-atopic healthy control subjects. We adjusted for cell-type composition in our models and used genome-wide and candidate-gene approaches. Results: We replicated one CpG which was significantly differentially methylated by severity, with suggestive replication at four others showing differential methylation by phenotype or severity. Not adjusting for eosinophil content, we identified 490 significantly differentially methylated CpGs (ADEH+ vs healthy controls, genome-wide). Many of these associated with severity measures, especially eosinophil count (431/490 sites). Conclusions: We identified a CpG in IL4 associated with serum tIgE levels, supporting a role for Th2 immune mediating mechanisms in AD. Changes in eosinophil level, a measure of disease severity, are associated with methylation changes, providing a potential mechanism for phenotypic changes in immune response-related traits.

KW - Atopic dermatitis

KW - DNA methylation

KW - Eczema herpeticum

KW - Human epigenetics

KW - Infinium Methylation 450K array

KW - Methylation EPIC array

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U2 - 10.1186/s13148-019-0714-1

DO - 10.1186/s13148-019-0714-1

M3 - Article

C2 - 31443688

AN - SCOPUS:85071510885

SN - 1868-7075

VL - 11

JO - Clinical Epigenetics

JF - Clinical Epigenetics

IS - 1

M1 - 122

ER -

Replicated methylation changes associated with eczema herpeticum and allergic response

Abstract

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