MHC class II stabilization at the surface of human dendritic cells is the result of maturation-dependent MARCH I down-regulation

Aude De Gassart(Inserm), Voahirana Camosseto(Inserm), Jacques Thibodeau(Institut National de la Recherche Scientifique), Maurizio Ceppi(Inserm), Nadia Catalan(Inserm), Philippe Pierre(Inserm), Evelina Gatti(Inserm)
Proceedings of the National Academy of Sciences
February 27, 2008
Cited by 248Open Access
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Abstract

In response to Toll-like receptor ligands, dendritic cells (DCs) dramatically enhance their antigen presentation capacity by stabilizing at the cell-surface MHC II molecules. We demonstrate here that, in human monocyte-derived DCs, the RING-CH ubiquitin E3 ligase, membrane-associated RING-CH I (MARCH I), promotes the ubiquitination of the HLA-DR beta-chain. Thus, in nonactivated DCs, MARCH I induces the surface internalization of mature HLA-DR complexes, therefore reducing their stability and levels. We further demonstrate that the maturation-dependent down-regulation of MARCH I is a key event in MHC class II up-regulation at the surface of LPS-activated DCs. MARCH I is, therefore, a major regulator of HLA-DR traffic, and its loss contributes to the acquisition of the potent immunostimulatory properties of mature human DCs.


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