| Literature DB >> 28147280 |
Florian Wanke1, Sonja Moos1, Andrew L Croxford1, André P Heinen1, Stephanie Gräf1, Bettina Kalt1, Denise Tischner2, Juan Zhang3, Isabelle Christen3, Julia Bruttger1, Nir Yogev1, Yilang Tang1, Morad Zayoud1, Nicole Israel1, Khalad Karram1, Sonja Reißig1, Sonja M Lacher1, Christian Reichhold1, Ilgiz A Mufazalov1, Avraham Ben-Nun4, Tanja Kuhlmann5, Nina Wettschureck2, Andreas W Sailer6, Klaus Rajewsky7, Stefano Casola8, Ari Waisman9, Florian C Kurschus10.
Abstract
Arrival of encephalitogenic T cells at inflammatory foci represents a critical step in development of experimental autoimmune encephalomyelitis (EAE), the animal model for multiple sclerosis. EBI2 and its ligand, 7α,25-OHC, direct immune cell localization in secondary lymphoid organs. CH25H and CYP7B1 hydroxylate cholesterol to 7α,25-OHC. During EAE, we found increased expression of CH25H by microglia and CYP7B1 by CNS-infiltrating immune cells elevating the ligand concentration in the CNS. Two critical pro-inflammatory cytokines, interleukin-23 (IL-23) and interleukin-1 beta (IL-1β), maintained expression of EBI2 in differentiating Th17 cells. In line with this, EBI2 enhanced early migration of encephalitogenic T cells into the CNS in a transfer EAE model. Nonetheless, EBI2 was dispensable in active EAE. Human Th17 cells do also express EBI2, and EBI2 expressing cells are abundant within multiple sclerosis (MS) white matter lesions. These findings implicate EBI2 as a mediator of CNS autoimmunity and describe mechanistically its contribution to the migration of autoreactive T cells into inflamed organs.Entities:
Keywords: 7α,25-OHC; CH25H; CNS; EAE; EBI2; GPR183; Th17; microglia; multiple sclerosis; oxysterol
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Year: 2017 PMID: 28147280 DOI: 10.1016/j.celrep.2017.01.020
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423