Lower prevalence of common filaggrin mutations in a community sample of atopic eczema: is disease severity important?

Lower prevalence of common filaggrin mutations in a community sample of atopic eczema: is disease severity important?

Summary BACKGROUND: Recent studies have shown an association of loss-of-function mutations in the filaggrin gene ( FLG ) with ichthyosis vulgaris and atopic eczema (AE). Case selection may have distorted the hitherto reported prevalence of FLG mutations and their relation to atopic disease. The aim...

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Veröffentlicht in:Wiener Klinische Wochenschrift 2010-10, Vol.122 (19-20), p.551-557
Hauptverfasser: Gruber, Robert, Janecke, Andreas R., Grabher, Daniela, Horak, Elisabeth, Schmuth, Matthias, Lercher, Peter
Format: Artikel
Sprache:eng
Schlagworte:
Austria - epidemiology
Child
Dermatitis, Atopic - classification
Dermatitis, Atopic - epidemiology
Dermatitis, Atopic - genetics
Endocrinology
Female
Gastroenterology
Genetic Predisposition to Disease - classification
Genetic Predisposition to Disease - epidemiology
Genetic Predisposition to Disease - genetics
Humans
Intermediate Filament Proteins - genetics
Internal Medicine
Male
Medicine
Medicine & Public Health
Mutation - genetics
Original Article
Pneumology/Respiratory System
Polymorphism, Single Nucleotide - genetics
Prevalence
Severity of Illness Index
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Zusammenfassung:Summary BACKGROUND: Recent studies have shown an association of loss-of-function mutations in the filaggrin gene ( FLG ) with ichthyosis vulgaris and atopic eczema (AE). Case selection may have distorted the hitherto reported prevalence of FLG mutations and their relation to atopic disease. The aim of the study was to determine the true population prevalence of FLG mutations in unselected children with and without reported physician diagnoses of asthma, allergic rhinitis and AE and their relationship with family history of atopic disease. METHODS: We used a nested case-control design by sampling children with reported doctor's diagnoses of AE, asthma and allergic rhinitis and randomly selected controls from a larger cross-sectional study ( n = 1263). Most common FLG mutations R501X, 2282del4, and R2447X were screened in DNA extracted from defrosted urine samples. The relationship of the combined FLG variants with atopic diseases and with reported family history of AE, asthma, and rhinitis was assessed. RESULTS: In the patient group one homozygote (R501X/R501X), 4 compound heterozygotes (3 R501X/2282del4, one 2282del4/R2447X), and 17 heterozygotes (10 R501X/wt, 5 2282del4/wt, and 2 R2447X/wt), in the control group 9 heterozygotes (5 R501X/wt, 4 2282del4/wt) were detected. The combined prevalence of FLG loss-of-function alleles was 5% in the control group and 9% in the atopic sample. In a subgroup analysis, the combination of allergic rhinitis and AE showed a significant relationship with FLG mutations, OR = 3.7 (1.01–12.67, p = 0.024). Likewise, significant relations with reported family history of asthma, OR = 4.35 (1.78–10.62, p = 0.0012), allergic rhinitis, OR = 2.33 (1.49–3.63, p = 0.0002), and AE, OR = 5.08 (2.78–9.30, p ≤ 0.0001) were observed. In contrast to clinical studies with higher percentages of severely affected persons, FLG mutations here showed a moderate association with atopic disease. CONCLUSIONS: Case selection may be responsible for overestimating the prevalence of FLG mutations in atopic disease.
ISSN:0043-5325
1613-7671
DOI:10.1007/s00508-010-1449-3