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Citations to this article

S1PR1 inhibition induces proapoptotic signaling in T cells and limits humoral responses within lymph nodes
Dhaval Dixit, … , Jordan E. Axelrad, Susan R. Schwab
Dhaval Dixit, … , Jordan E. Axelrad, Susan R. Schwab
Published January 9, 2024
Citation Information: J Clin Invest. 2024;134(4):e174984. https://doi.org/10.1172/JCI174984.
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Research Article Immunology Article has an altmetric score of 3

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

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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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Total citations by year

Year: 2025 2024 Total
Citations: 5 3 8
Citation information
This citation data is accumulated from CrossRef, which receives citation information from participating publishers, including this journal. Not all publishers participate in CrossRef, so this information is not comprehensive. Additionally, data may not reflect the most current citations to this article, and the data may differ from citation information available from other sources (for example, Google Scholar, Web of Science, and Scopus).

Citations to this article (8)

Title and authors Publication Year
Modulating lipid metabolism improves tumor immunotherapy
Ping Y, Fan Q, Zhang Y
Journal for Immunotherapy of Cancer 2025
Regulatory role of S1P and its receptors in sepsis-induced liver injury
Wang B, Wu X, Cheng J, Ye J, Zhu H, Liu X
Frontiers in Immunology 2025
Transcriptomics, lipidomics, and single-nucleus RNA sequencing integration: exploring sphingolipids in MASH-HCC progression
Zeng J, Way G, Wu N, Jiang X, Tai YL, Zhao D, Su L, Yan Q, Wang X, Gurley EC, Hylemon PB, Aseem SO, Sanyal AJ, Fan J, Zhou H
Cell & Bioscience 2025
Regulatory T cell and endothelial cell crosstalk.
Piao W, Lee ZL, Zapas G, Wu L, Jewell CM, Abdi R, Bromberg JS
Nature reviews. Immunology 2025
Aberrant T follicular helper cells generated by T(H)17 cell plasticity in the gut promote extraintestinal autoimmunity.
Fan T, Tai C, Sleiman KC, Cutcliffe MP, Kim H, Liu Y, Li J, Xin G, Grashel M, Baert L, Ekeocha C, Vergenes P, Lima S, Lo WL, Lin J, Hanaoka B, Tankersley TN, Wang M, Zhang X, Tsokos GC, Jarjour W, Longman R, Wu HJ
Nature immunology 2025
Discovery of Potent, Orally Bioavailable Sphingosine-1-Phosphate Transporter (Spns2) Inhibitors
Foster DJ, Dunnavant K, Shrader CW, LoPresti M, Seay S, Kharel Y, Brown AM, Huang T, Lynch KR, Santos WL
Journal of Medicinal Chemistry 2024
Regulation of cellular and systemic sphingolipid homeostasis.
Kuo A, Hla T
Nature reviews. Molecular cell biology 2024
Rapid determination of sphingosine 1-phosphate association with carrier molecules by flow-induced dispersion analysis to predict sepsis outcome
Seidita I, Ziegler A, Qalaj A, Winkler MS, Nierhaus A, Kluge S, Levkau B, Gräler MH
iScience 2024

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