Author: Martinâ€Blondel, Guillaume; Pignolet, Béatrice; Tietz, Silvia; Yshii, Lidia; Gebauer, Christina; Perinat, Therese; Van Weddingen, Isabelle; Blatti, Claudia; Engelhardt, Britta; Liblau, Roland
Title: Migration of encephalitogenic CD8 T cells into the central nervous system is dependent on the α4β1â€integrin Cord-id: 3q564wsb Document date: 2015_10_6
ID: 3q564wsb
Snippet: Although CD8 T cells are key players in neuroinflammation, little is known about their trafficking cues into the central nervous system (CNS). We used a murine model of CNS autoimmunity to define the molecules involved in cytotoxic CD8 Tâ€cell migration into the CNS. Using a panel of mAbs, we here show that the α4β1â€integrin is essential for CD8 Tâ€cell interaction with CNS endothelium. We also investigated which α4β1â€integrin ligands expressed by endothelial cells are implicated. The
Document: Although CD8 T cells are key players in neuroinflammation, little is known about their trafficking cues into the central nervous system (CNS). We used a murine model of CNS autoimmunity to define the molecules involved in cytotoxic CD8 Tâ€cell migration into the CNS. Using a panel of mAbs, we here show that the α4β1â€integrin is essential for CD8 Tâ€cell interaction with CNS endothelium. We also investigated which α4β1â€integrin ligands expressed by endothelial cells are implicated. The blockade of VCAMâ€1 did not protect against autoimmune encephalomyelitis, and only partly decreased the CD8(+) Tâ€cell infiltration into the CNS. In addition, inhibition of junctional adhesion moleculeâ€B expressed by CNS endothelial cells also decreases CD8 Tâ€cell infiltration. CD8 T cells may use additional and possibly unidentified adhesion molecules to gain access to the CNS.
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