Sialomucin CD 43 regulates T helper type 17 cell intercellular adhesion molecule 1 dependent adhesion, apical migration and transendothelial migration

FE Velázquez, M Anastasiou, FJ Carrillo‐Salinas… - …, 2019 - Wiley Online Library
FE Velázquez, M Anastasiou, FJ Carrillo‐Salinas, N Ngwenyama, AM Salvador, T Nevers…
Immunology, 2019Wiley Online Library
T helper type 17 lymphocytes (Th17 cells) infiltrate the central nervous system (CNS), induce
inflammation and demyelination and play a pivotal role in the pathogenesis of multiple
sclerosis. Sialomucin CD 43 is highly expressed in Th17 cells and mediates adhesion to
endothelial selectin (E‐selectin), an initiating step in Th17 cell recruitment to sites of
inflammation. CD 43−/− mice have impaired Th17 cell recruitment to the CNS and are
protected from experimental autoimmune encephalomyelitis (EAE), the mouse model of …
Summary
T helper type 17 lymphocytes (Th17 cells) infiltrate the central nervous system (CNS), induce inflammation and demyelination and play a pivotal role in the pathogenesis of multiple sclerosis. Sialomucin CD43 is highly expressed in Th17 cells and mediates adhesion to endothelial selectin (E‐selectin), an initiating step in Th17 cell recruitment to sites of inflammation. CD43−/− mice have impaired Th17 cell recruitment to the CNS and are protected from experimental autoimmune encephalomyelitis (EAE), the mouse model of multiple sclerosis. However, E‐selectin is dispensable for the development of EAE, in contrast to intercellular and vascular cell adhesion molecules (ICAM‐1 and VCAM‐1). We report that CD43−/− mice have decreased demyelination and T‐cell infiltration, but similar up‐regulation of ICAM‐1 and VCAM‐1 in the spinal cord, compared with wild‐type (WT) mice, at the initiation of EAE. CD43−/− Th17 cells have impaired adhesion to ICAM‐1 under flow conditions in vitro, despite having similar expression of LFA‐1, the main T‐cell ligand for ICAM‐1, as WT Th17 cells. Regardless of the route of integrin activation, CD43−/− Th17 cell firm arrest on ICAM‐1 was comparable to that of WT Th17 cells, but CD43−/− Th17 cells failed to optimally apically migrate on immobilized ICAM‐1‐coated coverslips and endothelial cells, and to transmigrate under shear flow conditions in an ICAM‐1‐dependent manner. Collectively, these findings unveil novel roles for CD43, facilitating adhesion of Th17 cells to ICAM‐1 and modulating apical and transendothelial migration, as mechanisms potentially responsible for Th17 cell recruitment to sites of inflammation such as the CNS.
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