Epithelial Inflammation Resulting from an Inherited Loss-of-function Mutation in EGFR

Overview

Journal J Invest Dermatol

Publisher Elsevier

Specialty Dermatology

Date 2014 Apr 3

PMID 24691054

Citations 40

Authors

Patrick Campbell

Penny E Morton

Takuya Takeichi

Amr Salam

Nerys Roberts

Laura E Proudfoot

Jemima E Mellerio

Kingi Aminu

Cheryl Wellington

Sachin N Patil

Masashi Akiyama

Lu Liu

James R McMillan

Sophia Aristodemou

Akemi Ishida-Yamamoto

Alya Abdul-Wahab

Gabriela Petrof

Kenneth Fong

Sarawin Harnchoowong

Kristina L Stone

John I Harper

W H Irwin McLean

Michael A Simpson

Maddy Parsons

John A McGrath

Affiliations

Soon will be listed here.

Abstract

Epidermal growth factor receptor (EGFR) signaling is fundamentally important for tissue homeostasis through EGFR/ligand interactions that stimulate numerous signal transduction pathways. Aberrant EGFR signaling has been reported in inflammatory and malignant diseases, but thus far no primary inherited defects in EGFR have been recorded. Using whole-exome sequencing, we identified a homozygous loss-of-function missense mutation in EGFR (c.1283 G>A; p.Gly428Asp) in a male infant with lifelong inflammation affecting the skin, bowel, and lungs. During the first year of life, his skin showed erosions, dry scale, and alopecia. Subsequently, there were numerous papules and pustules--similar to the rash seen in patients receiving EGFR inhibitor drugs. Skin biopsy demonstrated an altered cellular distribution of EGFR in the epidermis with reduced cell membrane labeling, and in vitro analysis of the mutant receptor revealed abrogated EGFR phosphorylation and EGF-stimulated downstream signaling. Microarray analysis on the patient's skin highlighted disturbed differentiation/premature terminal differentiation of keratinocytes and upregulation of several inflammatory/innate immune response networks. The boy died at the age of 2.5 years from extensive skin and chest infections as well as electrolyte imbalance. This case highlights the major mechanism of epithelial dysfunction following EGFR signaling ablation and illustrates the broader impact of EGFR inhibition on other tissues.

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