Atopic dermatitis phenotype affects expression of atopic diseases despite similar mononuclear cell cytokine response - 25/04/24

Doi : 10.1016/j.jaci.2024.02.015

Mohamed H. Taki, MD ^a,^b, Kristine E. Lee, MS ^c, Ronald Gangnon, PhD ^c, James E. Gern, MD ^a,^b, Robert F. Lemanske, MD ^a,^b, Daniel J. Jackson, MD ^a,^⁎ , Anne Marie Singh, MD ^a,^⁎
^a Department of Pediatrics, University of Wisconsin School of Medicine and Public Health, Madison, Wis
^b Department of Medicine, University of Wisconsin School of Medicine and Public Health, Madison, Wis
^c Department of Biostatistics and Medical Informatics, University of Wisconsin School of Medicine and Public Health, Madison, Wis

^∗Corresponding authors: Anne Marie Singh, MD, or Daniel J. Jackson, MD, 600 Highland Ave, K4/916, Madison, WI 53792.600 Highland AveK4/916MadisonWI53792

Sous presse. Épreuves corrigées par l'auteur. Disponible en ligne depuis le Thursday 25 April 2024

Abstract

Background

The atopic march refers to the coexpression and progression of atopic diseases in childhood, often beginning with atopic dermatitis (AD), although children may not progress through each atopic disease.

Objective

We hypothesized that future atopic disease expression is modified by AD phenotype and that these differences result from underlying dysregulation of cytokine signaling.

Methods

Children (n = 285) were enrolled into the Childhood Origins of Asthma (COAST) birth cohort and followed prospectively. Rates of AD, food allergy, allergic rhinitis, and asthma were assessed longitudinally from birth to 18 years of age. Associations between AD phenotype and food allergy, allergic rhinitis, asthma, allergic sensitization, exhaled nitric oxide, and lung function were determined. Peripheral blood mononuclear cell responses (IL-5, IL-10, IL-13, IFN-γ) to dust mite, phytohemagglutinin, Staphylococcus aureus Cowan I, and tetanus toxoid were compared among AD phenotypes.

Results

AD at year 1 was associated with an increased risk of food allergy (P = .004). Both persistent and late-onset AD were associated with an increased risk of asthma (P < .001), rhinitis (P < .001), elevated total IgE (P < .001), percentage of aeroallergens with detectable IgE (P < .001), and elevated exhaled nitric oxide (P = .002). Longitudinal analyses did not reveal consistent differences in peripheral blood mononuclear cell responses among dermatitis phenotypes.

Conclusion

AD phenotype is associated with differential expression of other atopic diseases. Our findings suggest that peripheral blood cytokine dysregulation is not a mechanism underlying this process, and immune dysregulation may be mediated at mucosal surfaces or in secondary lymphoid organs.

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Key words : Atopic dermatitis, atopic march, atopic dermatitis phenotypes, allergic sensitization, progression of atopic disease

Abbreviations used : AD, CCL, COAST, Feno, FEV₁, FVC, PBMC, TSLP