Please use this identifier to cite or link to this item: https://hdl.handle.net/20.500.14279/1498
Title: FTY720 blocks egress of T cells in part by abrogation of their adhesion on the lymph node sinus
Authors: Zhi, Liang 
Kim, Pilhan 
Pitsillides, Costas 
Major Field of Science: Medical and Health Sciences
Field Category: Health Sciences
Keywords: Immunology;T cells;Lymph nodes;Mice;Animal experimentation;Cell adhesion
Issue Date: 2011
Source: Journal of immunology, 2011, vol. 187, no. 5, pp. 2244-2251
Volume: 187
Issue: 5
Start page: 2244
End page: 2251
Journal: The Journal of Immunology 
Abstract: Egress of lymphocytes from lymphoid tissues is a complex process in which Gαi-mediated signals play a decisive role. We show here that although FTY720, an agonist of the sphingosine 1-phosphate (S1P)1 receptor, induces S1P1 receptor internalization sufficiently in the presence or absence of Gαi2 or Gαi3, the drug blocks egress of wild-type (WT) and Gαi3-deficent T cells, but not Gαi2-deficient T cells, in both WT and Gαi2-deficient hosts. Intravital imaging of lymph nodes revealed that all three groups of T cells approached and engaged cortical sinusoids similarly in the presence or absence of FTY720. The cells also entered and departed the sinus at an almost identical frequency in the absence of the drug. However, after engagement of the sinus, most WT and Gαi3-deficient T cells retracted and migrated back into the parenchyma in FTY720-treated animals, due to a failure of the cells to establish adhesion on the sinus, whereas Gαi2-deficient T cells adhered firmly on the sinus, which prevented their retraction, facilitating their transmigration of the lymphatic endothelial barrier. These data confirm egress of Gαi2−/− T cells independent of S1P-mediated chemotaxis and failure of FTY720 to close lymphatic stromal channels and argue for the first time, to our knowledge, that FTY720 induces lymphopenia in part by impairing T cell adhesion to the sinus in a manner dependent on Gαi2
URI: https://hdl.handle.net/20.500.14279/1498
ISSN: 15506606
DOI: 10.4049/jimmunol.1100670
Rights: © American Association of Immunologists
Type: Article
Affiliation: Massachusetts General Hospital 
Affiliation : Cyprus University of Technology 
Massachusetts General Hospital 
Korea Advanced Institute of Science & Technology 
Publication Type: Peer Reviewed
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