Increased Serine Protease Activity and Cathelicidin Promotes Skin Inflammation in Rosacea

Overview

Journal Nat Med

Specialties General Medicine
Molecular Biology

Date 2007 Aug 7

PMID 17676051

Citations 253

Authors

Kenshi Yamasaki

Anna Di Nardo

Antonella Bardan

Masamoto Murakami

Takaaki Ohtake

Alvin Coda

Robert A Dorschner

Chrystelle Bonnart

Pascal Descargues

Alain Hovnanian

Vera B Morhenn

Richard L Gallo

Affiliations

Soon will be listed here.

Abstract

Acne rosacea is an inflammatory skin disease that affects 3% of the US population over 30 years of age and is characterized by erythema, papulopustules and telangiectasia. The etiology of this disorder is unknown, although symptoms are exacerbated by factors that trigger innate immune responses, such as the release of cathelicidin antimicrobial peptides. Here we show that individuals with rosacea express abnormally high levels of cathelicidin in their facial skin and that the proteolytically processed forms of cathelicidin peptides found in rosacea are different from those present in normal individuals. These cathelicidin peptides are a result of a post-translational processing abnormality associated with an increase in stratum corneum tryptic enzyme (SCTE) in the epidermis. In mice, injection of the cathelicidin peptides found in rosacea, addition of SCTE, and increasing protease activity by targeted deletion of the serine protease inhibitor gene Spink5 each increases inflammation in mouse skin. The role of cathelicidin in enabling SCTE-mediated inflammation is verified in mice with a targeted deletion of Camp, the gene encoding cathelicidin. These findings confirm the role of cathelicidin in skin inflammatory responses and suggest an explanation for the pathogenesis of rosacea by demonstrating that an exacerbated innate immune response can reproduce elements of this disease.

Citing Articles

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