Meta-analysis Confirms the LCE3C_LCE3B Deletion As a Risk Factor for Psoriasis in Several Ethnic Groups and Finds Interaction with HLA-Cw6

Overview

Journal J Invest Dermatol

Publisher Elsevier

Specialty Dermatology

Date 2010 Nov 26

PMID 21107349

Citations 44

Authors

Eva Riveira-Munoz

Su-Min He

Georgia Escaramis

Philip E Stuart

Ulrike Huffmeier

Catherine Lee

Brian Kirby

Akira Oka

Emiliano Giardina

Wilson Liao

Judith Bergboer

Kati Kainu

Rafael de Cid

Batmunkh Munkhbat

Patrick L J M Zeeuwen

John A L Armour

Annie Poon

Tomotaka Mabuchi

Akira Ozawa

Agnieszka Zawirska

A David Burden

Jonathan N Barker

Francesca Capon

Heiko Traupe

Liang-Dan Sun

Yong Cui

Xian-Yong Yin

Gang Chen

Henry W Lim

Rajan P Nair

John J Voorhees

Trilokraj Tejasvi

Ramon Pujol

Namid Munkhtuvshin

Judith Fischer

Juha Kere

Joost Schalkwijk

Anne Bowcock

Pui-Yan Kwok

Giuseppe Novelli

Hidetoshi Inoko

Anthony W Ryan

Richard C Trembath

Andre Reis

Xue-Jun Zhang

James T Elder

Xavier Estivill

Affiliations

Soon will be listed here.

Abstract

A multicenter meta-analysis including data from 9,389 psoriasis patients and 9,477 control subjects was performed to investigate the contribution of the deletion of genes LCE3C and LCE3B, involved in skin barrier defense, to psoriasis susceptibility in different populations. The study confirms that the deletion of LCE3C and LCE3B is a common genetic factor for susceptibility to psoriasis in the European populations (OR(Overall) = 1.21 (1.15-1.27)), and for the first time directly demonstrates the deletion's association with psoriasis in the Chinese (OR = 1.27 (1.16-1.34)) and Mongolian (OR = 2.08 (1.44-2.99)) populations. The analysis of the HLA-Cw6 locus showed significant differences in the epistatic interaction with the LCE3C and LCE3B deletion in at least some European populations, indicating epistatic effects between these two major genetic contributors to psoriasis. The study highlights the value of examining genetic risk factors in multiple populations to identify genetic interactions, and indicates the need of further studies to understand the interaction of the skin barrier and the immune system in susceptibility to psoriasis.

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