S1PR1 inhibition induces proapoptotic signaling in T cells and limits humoral responses within lymph nodes
Dhaval Dixit, Victoria M. Hallisey, Ethan Y.S. Zhu, Martyna Okuniewska, Ken Cadwell, Jerry E. Chipuk, Jordan E. Axelrad, Susan R. Schwab
Dhaval Dixit, Victoria M. Hallisey, Ethan Y.S. Zhu, Martyna Okuniewska, Ken Cadwell, Jerry E. Chipuk, Jordan E. Axelrad, Susan R. Schwab
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Research Article Immunology

S1PR1 inhibition induces proapoptotic signaling in T cells and limits humoral responses within lymph nodes

Abstract

Effective immunity requires a large, diverse naive T cell repertoire circulating among lymphoid organs in search of antigen. Sphingosine 1-phosphate (S1P) and its receptor S1PR1 contribute by both directing T cell migration and supporting T cell survival. Here, we addressed how S1P enables T cell survival and the implications for patients treated with S1PR1 antagonists. We found that S1PR1 limited apoptosis by maintaining the appropriate balance of BCL2 family members via restraint of JNK activity. Interestingly, the same residues of S1PR1 that enable receptor internalization were required to prevent this proapoptotic cascade. Findings in mice were recapitulated in ulcerative colitis patients treated with the S1PR1 antagonist ozanimod, and the loss of naive T cells limited B cell responses. Our findings highlighted an effect of S1PR1 antagonists on the ability to mount immune responses within lymph nodes, beyond their effect on lymph node egress, and suggested both limitations and additional uses of this important class of drugs.

Authors

Dhaval Dixit, Victoria M. Hallisey, Ethan Y.S. Zhu, Martyna Okuniewska, Ken Cadwell, Jerry E. Chipuk, Jordan E. Axelrad, Susan R. Schwab

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Figure 6

GRK2 regulates naive T cell survival.

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GRK2 regulates naive T cell survival. (A) CD45.1/2 WT mice were lethally...
(A) CD45.1/2 WT mice were lethally irradiated and reconstituted with either Grk2fl/– Cd4-Cre (Grk2Δ) or Grk2fl/+ Cd4-Cre (ctrl) bone marrow. Eight to twelve weeks after bone marrow transfer, naive T cells were analyzed. (B and C) Representative histogram of surface S1PR1 on naive CD4+ T cells in blood (B), and compilation (C). (D) Frequency of ActCasp+ annexin V+ cells among naive CD4+ T cells in LNs. (E and F) Relative MFI values for p-MKK7 and p-JNK (E) and for BCL2, PUMA, and BAX (F). Relative values represent expression in 1 mouse divided by the mean for littermate controls in that experiment. Compilation of 4 experiments, 6–7 per group. Student’s t test. *P ≤ 0.05, **P ≤ 0.01, ***P ≤ 0.001, ****P ≤ 0.0001.