1. NFAT signaling is indispensable for persistent memory responses of MCMV-specific CD8+ T cells.
- Author
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Chaudhry, M. Zeeshan, Borkner, Lisa, Kulkarni, Upasana, Berberich-Siebelt, Friederike, and Cicin-Sain, Luka
- Subjects
T cells ,T cell receptors ,CELL analysis ,GRAFT rejection ,VIRUS reactivation ,IMMUNOSENESCENCE ,IMMUNOSUPPRESSIVE agents - Abstract
Cytomegalovirus (CMV) induces a unique T cell response, where antigen-specific populations do not contract, but rather inflate during viral latency. It has been proposed that subclinical episodes of virus reactivation feed the inflation of CMV-specific memory cells by intermittently engaging T cell receptors (TCRs), but evidence of TCR engagement has remained lacking. Nuclear factor of activated T cells (NFAT) is a family of transcription factors, where NFATc1 and NFATc2 signal downstream of TCR in mature T lymphocytes. We show selective impacts of NFATc1 and/or NFATc2 genetic ablations on the long-term inflation of MCMV-specific CD8
+ T cell responses despite largely maintained responses to acute infection. NFATc1 ablation elicited robust phenotypes in isolation, but the strongest effects were observed when both NFAT genes were missing. CMV control was impaired only when both NFATs were deleted in CD8+ T cells used in adoptive immunotherapy of immunodeficient mice. Transcriptome analyses revealed that T cell intrinsic NFAT is not necessary for CD8+ T cell priming, but rather for their maturation towards effector-memory and in particular the effector cells, which dominate the pool of inflationary cells. Author summary: Cytomegalovirus (CMV) infection is a very common cause of complications in transplant recipients. These patients suffer from opportunistic viruses because their immune system is weakened by immunosuppressive drugs, which are required to avoid transplant rejection by T cells, a key lymphocyte population involved in antiviral defenses. The commonly used immunosuppressive drugs target gene products in a signaling pathway inside T lymphocytes involving two Nuclear Factors of Activated T cells (NFAT) called NFATc1 and NFATc2. We tested the effects of NFAT signaling on T cell responses to CMV in mice lacking either of these genes, or both of them. We show that the T cell responses to CMV are compromised in absence of NFATc1 in a peculiar manner. While early responses upon infection are robust, they are not maintained in the long term. A detailed analysis of these cells showed that cells lacking NFAT display a deficit in T-cell maturation upon the initial activation. Our data may have relevance for the design of future immunosuppressive drugs that may protect patients from organ rejection, while retaining antiviral immune defenses. [ABSTRACT FROM AUTHOR]- Published
- 2024
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