Whole genome sequencing identifies genetic variants associated with neurogenic inflammation in rosacea

Author:

Deng ZhiliORCID,Chen MengtingORCID,Zhao Zhixiang,Xiao Wenqin,Liu Tangxiele,Peng Qinqin,Wu Zheng,Xu San,Shi Wei,Jian Dan,Wang Ben,Liu Fangfen,Tang Yan,Huang Yingxue,Zhang Yiya,Wang Qian,Sun LunquanORCID,Xie Hongfu,Zhang GuohongORCID,Li JiORCID

Abstract

AbstractRosacea is a chronic inflammatory skin disorder with high incidence rate. Although genetic predisposition to rosacea is suggested by existing evidence, the genetic basis remains largely unknown. Here we present the integrated results of whole genome sequencing (WGS) in 3 large rosacea families and whole exome sequencing (WES) in 49 additional validation families. We identify single rare deleterious variants of LRRC4, SH3PXD2A and SLC26A8 in large families, respectively. The relevance of SH3PXD2A, SLC26A8 and LRR family genes in rosacea predisposition is underscored by presence of additional variants in independent families. Gene ontology analysis suggests that these genes encode proteins taking part in neural synaptic processes and cell adhesion. In vitro functional analysis shows that mutations in LRRC4, SH3PXD2A and SLC26A8 induce the production of vasoactive neuropeptides in human neural cells. In a mouse model recapitulating a recurrent Lrrc4 mutation from human patients, we find rosacea-like skin inflammation, underpinned by excessive vasoactive intestinal peptide (VIP) release by peripheral neurons. These findings strongly support familial inheritance and neurogenic inflammation in rosacea development and provide mechanistic insight into the etiopathogenesis of the condition.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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