2016
DOI: 10.1073/pnas.1516485113
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T cell-intrinsic S1PR1 regulates endogenous effector T-cell egress dynamics from lymph nodes during infection

Abstract: Viral clearance requires effector T-cell egress from the draining lymph node (dLN). The mechanisms that regulate the complex process of effector T-cell egress from the dLN after infection are poorly understood. Here, we visualized endogenous pathogen-specific effector T-cell migration within, and from, the dLN. We used an inducible mouse model with a temporally disrupted sphingosine-1-phosphate receptor-1 (S1PR1) gene specifically in endogenous effector T cells. Early after infection, WT and S1PR1 −/− effector… Show more

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Cited by 69 publications
(76 citation statements)
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“…Although it is possible that FTY720 might also act on other S1P receptors, such as S1P3, S1P4, and S1P5, the Ex26 compound is a selective S1P1 receptor antagonist, confirming the relevance of this receptor in the outcome of P. aeruginosa infection. Notably, treatment with either Ex26 or FTY720 results in alteration of trafficking and egress of lymphocytes (27,38), and lymphocyte egress is mediated by S1P1 activity (39). In addition, in another study, sphingosine was involved in pulmonary infection in mice with burn injuries (40), suggesting that S1P1 may also have a role during P. aeruginosa infection processes, as indicated by our results.…”
Section: Discussionsupporting
confidence: 69%
“…Although it is possible that FTY720 might also act on other S1P receptors, such as S1P3, S1P4, and S1P5, the Ex26 compound is a selective S1P1 receptor antagonist, confirming the relevance of this receptor in the outcome of P. aeruginosa infection. Notably, treatment with either Ex26 or FTY720 results in alteration of trafficking and egress of lymphocytes (27,38), and lymphocyte egress is mediated by S1P1 activity (39). In addition, in another study, sphingosine was involved in pulmonary infection in mice with burn injuries (40), suggesting that S1P1 may also have a role during P. aeruginosa infection processes, as indicated by our results.…”
Section: Discussionsupporting
confidence: 69%
“…The most down-regulated genes were notable for several chemokine receptors (S1pr1, Cxcr5, Ccr7) and other genes typically expressed at low levels in effector CD8 + T cells (Il7r, Actn1) ( Fig. 5A) [33,34]. These data suggest that IL- 10 + hepatic CD8 + T cells are programmed to circulate through nonlymphoid tissues, consistent with their accumulation in the liver.…”
Section: Il-10 + Hepatic Cd8 + T Cells Possess a Distinct Transcriptimentioning
confidence: 75%
“…S1PR1 is thought to regulate naive lymphocyte egress from the lymph node via the lymphatic vessels by sealing the lymphatic endothelial barrier and disallowing naive T cell egress from lymph node and thymus (Alfonso, McHeyzer-Williams, & Rosen, 2006;Sanna et al, 2006). Egress is a more complex process than just sensing of the ligand S1P (Cyster & Schwab, 2012) that is present in high quantities in the lymph (Benechet et al, 2016). Once lymphocytes reach circulation, the surface expression of S1PR1 is rapidly downregulated (Lo, Xu, Proia, & Cyster, 2005) as a result of the high amounts of S1P in the lymph and blood (Pappu et al, 2007).…”
Section: Discussionmentioning
confidence: 99%