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The sphingosine-1-phosphate receptor agonist FTY720 modulates dendritic cell trafficking in vivo. | LitMetric

The sphingosine-1-phosphate receptor agonist FTY720 modulates dendritic cell trafficking in vivo.

Am J Transplant

Thomas E. Starzl Transplantation Institute and Department of Surgery, University of Pittsburgh, Pittsburgh, Pennsylvania, USA.

Published: November 2005

AI Article Synopsis

  • FTY720 is a pro-drug in phase III trials aimed at preventing organ rejection by inhibiting lymphocyte movement through its action on S1PR1 receptors.
  • In a study, FTY720 treatment in mice led to a decrease in circulating T and B lymphocytes but an increase in blood-borne dendritic cells (DCs), while DCs in lymph nodes and the spleen decreased.
  • The research suggests that FTY720's effects on DC trafficking may enhance its capability to suppress the immune response, which could influence its potential effectiveness in organ transplant scenarios.

Article Abstract

The pro-drug FTY720 is undergoing phase III clinical trials for prevention of allograft rejection. After phosphorylation, FTY720 targets the G protein-coupled-sphingosine-1-phosphate receptor 1 (S1PR1) on lymphocytes, thereby inhibiting their egress from lymphoid organs and their recirculation to inflammatory sites. Potential effects on dendritic cell (DC) trafficking have not been evaluated. Here, we demonstrate the expression of all five S1PR subtypes (S1PR1-5) by murine DCs. Administration of FTY720 to C57BL/10 mice markedly reduced circulating T and B lymphocytes within 24 h, but not blood-borne DCs, which were enhanced significantly for up to 96 h, while DCs in lymph nodes and spleen were reduced. Numbers of adoptively transferred, fluorochrome-labeled syngeneic or allogeneic DCs in blood were increased significantly in FTY720-treated animals, while donor-derived DCs and allostimulatory activity for host naïve T cells within the spleen were reduced. Administration of the selective S1PR1 agonist SEW2871 significantly enhanced circulating DC numbers. Flow analysis revealed that CD11b, CD31/PECAM-1, CD54/ICAM-1 and CCR7 expression on blood-borne DCs was downregulated following FTY720 administration. Transendothelial migration of FTY720-P-treated immature DCs to the CCR7 ligand CCL19 was reduced. These novel data suggest that modulation of DC trafficking by FTY720 may contribute to its immunosuppressive effects.

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Source
http://dx.doi.org/10.1111/j.1600-6143.2005.01085.xDOI Listing

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