Pivotal role of CD103 in the development of psoriasiform dermatitis

Takehito Fukui,Yotaro Nishikawa,Haruhiko Koseki,Yoshitaka Hishikawa,Narantsog Choijookhuu,Yoshihiro Yamashita,Junta Nasu,Tomohiro Fukaya,Hideaki Takagi,Tomofumi Uto,Noriaki Miyanaga,Katsuaki Sato

doi:10.1038/s41598-020-65355-9

Abstract

The integrin αE known as CD103 binds integrin β7 to form the complete heterodimeric integrin molecule αEβ7. CD103 is mainly expressed by lymphocytes within epithelial tissues of intestine, lung, and skin as well as subsets of mucosal and dermal conventional dendritic cells (cDCs). CD103 has been originally implicated in the attachment of lymphocytes to epithelium in the gut and skin through the interaction with E-cadherin expressed on intestinal epithelial cells, keratinocytes, and Langerhans cells (LCs). However, an impact of CD103 on the cutaneous immune responses and the development of inflammatory skin diseases remains elusive. Here, we report that CD103 regulates the development of psoriasiform dermatitis through the control of the function of cDCs. Deficiency in CD103 exacerbates psoriasiform dermatitis, accompanied by excessive epidermal hyperplasia and infiltration of inflammatory leukocytes. Furthermore, deficiency in CD103 not only accelerates the production of proinflammatory cytokines in psoriatic lesions but also promotes the generation of lymphocytes producing interleukin (IL)-17 in the skin-draining peripheral lymph nodes (PLNs). Under the deficiency in CD103, cDCs localized in PLNs enhance cytokine production following activation. Thus, our findings reveal a pivotal role for CD103 in the control of the function of cDCs to regulate cutaneous inflammation in psoriasiform dermatitis.

Highlights

The integrin αE known as CD103 binds integrin β7 to form the complete heterodimeric integrin molecule αEβ7
CD103 has been originally implicated in the attachment of lymphocytes to epithelial tissues in the gut and skin through the interaction with E-cadherin expressed on intestinal epithelial cells, keratinocytes, and Langerhans cells (LCs)[17,18,19,20]
The accumulating evidences suggest that CD103 is involved in the pathogenesis of some immune-mediated diseases such as graft-versus-host diseases (GVHD), asthma, and allergic contact hypersensitivity, how CD103 controls immune responses leading to the development of cutaneous inflammatory disorders remains unclear

Summary

Introduction

The integrin αE known as CD103 binds integrin β7 to form the complete heterodimeric integrin molecule αEβ7. We report that CD103 regulates the development of psoriasiform dermatitis through the control of the function of cDCs. Deficiency in CD103 exacerbates psoriasiform dermatitis, accompanied by excessive epidermal hyperplasia and infiltration of inflammatory leukocytes. While CD103 has reportedly no obvious pathogenic role in psoriasiform skin lesions of transgenic (Tg) mice overexpressing human transforming growth factor (TGF)-β1 under the regulation of the keratin 5 promoter within the epidermis (K5.hTGFβ1 Tg mice), which displayed a spontaneous development of psoriatic dermatitis[29], the potential role of CD103 in the control of the pathogenesis of psoriasiform dermatitis and other cutaneous inflammatory disorders remains elusive. We show that impact of CD103 on the development of psoriasiform dermatitis mediated through the control of the function of cDCs in the skin-draining peripheral lymph nodes (PLNs) with use of CD103-deficient mice

Methods

Results

Conclusion