Filaggrin gene polymorphisms in Indian children with atopic dermatitis: A cross-sectional multicentre study

Author:

Srinivas Sahana M1,Dhar Sandipan2,Gowdra Aruna3,Saha Abhijit2,Sundararajan Lakshmi4,Geetha Thenral S4,Banerjee Raghubir2,Malakar Rajib2,Sil Amrita5,Lakshminarayana Shyam Prasad Arakali6

Affiliation:

1. Department of Pediatric Dermatology, Indira Gandhi Institute of Child Health, Bengaluru, Karnataka, India

2. Department of Pediatric Dermatology, Institute of Child Health, Kolkata, West Bengal, India

3. Department of Microbiology, Indira Gandhi Institute of Child Health, Bengaluru, Karnataka, India

4. MedGenome Labs Ltd., Bengaluru, Karnataka, India

5. Department of Pharmacology, Rampurhat Government Medical College and Hospital, Birbhum, West Bengal, India

6. Department of Dermatology, Ramaiah Medical College and Hospital, Bengaluru, Karnataka, India,

Abstract

Background Filaggrin (FLG) gene encoding the protein filaggrin plays an important role in barrier function of the skin and its alteration is a predisposing factor for atopic dermatitis. FLG gene variants result in absent or decreased filaggrin protein. Worldwide, the prevalence of FLG variants ranges from 14 to 56%. FLG null variants are distinct in each population. Objectives To study the FLG gene polymorphisms in Indian children and attempt a genotype-phenotype correlation in atopic dermatitis. Methods This was a cross-sectional, multicentre study conducted on 75 Indian children. Demographic details, clinical features and identified FLG null variants were recorded. We performed a whole gene sequencing of the entire FLG coding region using next-generation sequencing technology. Results The prevalence of FLG null variants was 34.7%. A total of 20 different FLG loss of function variants in 26 children were documented. Sixteen (80%) variants were novel and four (20%) were previously reported in Asian and European populations. We found a statistically significant association between FLG variants with early age of onset of atopic dermatitis (P = 0.016) and elevated serum IgE levels (P = 0.051). There was no significant difference between atopic dermatitis phenotypes in children having one variant as compared to children harbouring two or more null variants. Limitation Small sample size. Conclusion Our study reports a unique set of FLG variants different from Asian and European populations, with these variants being significantly associated with an early age of onset of atopic dermatitis and elevated serum IgE levels.

Publisher

Scientific Scholar

Subject

Infectious Diseases,Dermatology

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