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SPNS2 enables T cell egress from lymph nodes during an immune response

Martyna Okuniewska, Victoria Fang, Audrey Baeyens, Varsha Raghavan, June‐Yong Lee, Dan R. Littman, Susan R. Schwab

2021Cell Reports29 citationsDOIOpen Access PDF

Abstract

T cell expression of sphingosine 1-phosphate (S1P) receptor 1 (S1PR1) enables T cell exit from lymph nodes (LNs) into lymph, while endothelial S1PR1 expression regulates vascular permeability. Drugs targeting S1PR1 treat autoimmune disease by trapping pathogenic T cells within LNs, but they have adverse cardiovascular side effects. In homeostasis, the transporter SPNS2 supplies lymph S1P and enables T cell exit, while the transporter MFSD2B supplies most blood S1P and supports vascular function. It is unknown whether SPNS2 remains necessary to supply lymph S1P during an immune response, or whether in inflammation other compensatory transporters are upregulated. Here, using a model of dermal inflammation, we demonstrate that SPNS2 supplies the S1P that guides T cells out of LNs with an ongoing immune response. Furthermore, deletion of Spns2 is protective in a mouse model of multiple sclerosis. These results support the therapeutic potential of SPNS2 inhibitors to achieve spatially specific modulation of S1P signaling.

Topics & Concepts

S1PR1LymphImmune systemInflammationImmunologySphingosineSphingosine-1-phosphateT cellCell biologyDownregulation and upregulationMedicineBiologyReceptorCancer researchInternal medicinePathologyVascular endothelial growth factor AGeneVascular endothelial growth factorVEGF receptorsBiochemistrySphingolipid Metabolism and SignalingNeuroinflammation and Neurodegeneration MechanismsImmune cells in cancer
SPNS2 enables T cell egress from lymph nodes during an immune response | Litcius