Longitudinal atopic dermatitis endotypes: An atopic march paradigm that includes Black children - 04/05/22
Abstract |
Background |
The atopic march has been studied mostly in White populations, biasing our current paradigms.
Objective |
We sought to define the atopic march in Black and White children and explore mechanisms for racial differences.
Methods |
Utilizing the Mechanisms of Progression of Atopic Dermatitis to Asthma in Children (MPAACH) cohort (n = 601), we assessed longitudinal sensitization, food allergy (FA), allergic rhinitis, risk of asthma development (through the Pediatric Asthma Risk Score), Scoring for Atopic Dermatitis (SCORAD), transepidermal water loss, skin filaggrin (FLG) expression, exposures, and genetic heritability to define AD progression endotypes in Black and White children.
Results |
White MPAACH children were more likely to be sensitized to aero and food allergens (P = .0001) and over 3 times more likely to develop FA and/or allergic rhinitis (AR) without asthma risk (P < .0001). In contrast, Black children were over 6 times more likely to proceed to high asthma risk without FA, sensitization, or AR (P < .0001). White children had higher lesional and nonlesional transepidermal water loss (both P < .001) as well as decreased nonlesional keratinocyte FLG expression (P = .02). Black children had increased genetic heritability for asthma risk and higher rates of exposures to secondhand smoke and traffic-related air pollution.
Conclusions |
Black and White children with AD have distinct allergic trajectories defined by different longitudinal endotypes. Black children exhibit higher asthma risk despite a more intact skin barrier and less sensitization, FA, and AR. White children have less asthma risk, despite a more dysfunctional skin barrier, and more FA, AR, and sensitization. The observed racial differences are likely due in part to increased genetic heritability for asthma risk and harmful environmental exposures in Black children. Collectively, our findings provide a new paradigm for an atopic march that is inclusive of Black children.
Le texte complet de cet article est disponible en PDF.Graphical abstract |
Key words : Atopic march, atopic dermatitis, race, genetic ancestry, environmental exposure, skin barrier, biomarker
Abbreviations used : AD, AR, CCHMC, FA, FLG, IQR, MPAACH, PARS, SCORAD, SHS, SPT, TEWL, TRAP, V1/2
Plan
| This work was supported by National Institutes of Health grant U19AI070235 (G.K.H., J.M.B., L.J.M.). |
|
| Disclosure of potential conflict of interest: The authors declare that they have no relevant conflicts of interest. |
Vol 149 - N° 5
P. 1702 - mai 2022 Retour au numéro
Article précédent
- CD38+ B cells affect immunotherapy for allergic rhinitis
- Gui-Xiang Tian, Ke-Ping Peng, Ming-Hui Liu, Dao-Fa Tian, Hai-Qing Xie, Li-Wen Wang, Yu-Yang Guo, Shan Zhou, Li-Hua Mo, Ping-Chang Yang
- Mepolizumab for chronic rhinosinusitis with nasal polyps: Treatment efficacy by comorbidity and blood eosinophil count
- Claus Bachert, Ana R. Sousa, Joseph K. Han, Rodney J. Schlosser, Leigh J. Sowerby, Claire Hopkins, Jorge F. Maspero, Steven G. Smith, Oliver Kante, Despina E. Karidi-Andrioti, Bhabita Mayer, Robert H. Chan, Steve W. Yancey, Adam M. Chaker
Bienvenue sur EM-consulte, la référence des professionnels de santé.
L’accès au texte intégral de cet article nécessite un abonnement.
Déjà abonné à cette revue ?