Comorbidities in childhood atopic dermatitis: A population‐based study

Author:

von Kobyletzki Laura1ORCID,Henrohn Dan23ORCID,Ballardini Natalia456ORCID,Neary Maureen P.7ORCID,Ortsäter Gustaf8ORCID,Rieem Dun Alexander8ORCID,Geale Kirk89ORCID,Lindberg Ingrid8ORCID,Theodosiou Grigorios10ORCID,Neregård Petra2ORCID,De Geer Anna2ORCID,Cha Amy11ORCID,Cappelleri Joseph C.12ORCID,Thyssen Jacob P.13ORCID

Affiliation:

1. Department of Occupational and Environmental Dermatology Skåne University Hospital, Lund University Lund Sweden

2. Inflammation and Immunology Pfizer AB Stockholm Sweden

3. Department of Medical Sciences Uppsala University Uppsala Sweden

4. Institute of Environmental Medicine Karolinska Institutet Stockholm Sweden

5. Department of Dermatology and Sexual Health Södersjukhuset Stockholm Sweden

6. Department of Clinical Science and Education Södersjukhuset, Karolinska Institutet Stockholm Sweden

7. Inflammation and Immunology Pfizer Inc. Collegeville Pennsylvania USA

8. Quantify Research AB Stockholm Sweden

9. Dermatology and Venereology, Department of Public Health and Clinical Medicine Umeå University Umeå Sweden

10. Department of Dermatology Skåne University Hospital Malmö Sweden

11. Inflammation and Immunology Pfizer Inc. New York New York USA

12. Global Biometrics and Data Management (Statistics) Pfizer Inc. Groton Connecticut USA

13. Department of Dermatology and Venereology Bispebjerg Hospital, University of Copenhagen Copenhagen Denmark

Abstract

AbstractBackgroundAtopic dermatitis (AD) is a chronic inflammatory skin disease that is associated with allergic comorbidities. However, studies examining comorbidities in childhood AD are incomplete, which may contribute to suboptimal care.ObjectiveThe objective was to compare the risk of developing different allergic and non‐allergic comorbidities among children with AD to that of a matched non‐AD reference cohort in Sweden.MethodsThis was a nationwide population‐based cohort study using longitudinal data from primary and specialist care registers. Patients with AD were identified by confirmed diagnosis in primary or specialist care. The non‐AD reference cohort was randomly drawn from the general population and matched 1:1 with the AD patients. The risk of developing the following conditions was evaluated: hypersensitivity and allergic disorders, neurological disorders, psychiatric disorders, infections, immunological and inflammatory disorders, Type 1 diabetes (T1D), endocrine and metabolic disorders, skeletal disorders, ocular disorders and malignancies.ResultsThis study included 165,145 patients with AD (mild‐to‐moderate [n = 126,681] and severe [n = 38,464]) and an equally sized reference cohort. Patients with AD displayed a higher risk of developing comorbid conditions for all investigated categories, except for T1D and skeletal disorders, compared with the reference cohort. The highest risk compared with the reference cohort was observed for hypersensitivity and allergic disorders (hazard ratio [HR]: 3.87), followed by malignancies (HR: 2.53) and immunological and inflammatory disorders (HR: 2.36). Patients with AD also had higher risk of developing multiple comorbidities (≥2). The risk of comorbidity onset increased alongside AD severity and patients with active AD were associated with increased risk of comorbidity onset compared with patients in remission.ConclusionsThe clinical burden of AD is substantial for children with AD and patients are at an increased risk of developing several comorbid conditions extending beyond the atopic march. Our results also showed a positive association between worsening severity of AD and an increased risk of comorbidity onset.

Publisher

Wiley

Subject

Infectious Diseases,Dermatology

Reference51 articles.

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5. SilverbergJBS GadkariA SimpsonE WeidingerS Mina‐OsorioP RossiA et al.Epidemiology of atopic dermatitis in the adolescent population: a cross‐sectional study in the United States and Europe.2019.

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