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  5. Disruptors of sestrin-MAPK interactions rejuvenate T cells and expand TCR specificity

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Preprint
en
2024

Disruptors of sestrin-MAPK interactions rejuvenate T cells and expand TCR specificity

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en
2024
DOI: 10.1101/2024.05.17.594698dx.doi.org/10.1101/2024.05.17.594698

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Michael Karin
Michael Karin

University of California, San Diego

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Alessio Lanna
Clara D’Ambra
Federica Rinaldi
+4 more

Abstract

Summary Whereas treatments that reactivate exhausted T cells are available, strategies to rejuvenate terminally differentiated senescent lymphocytes are yet to be developed. Senescent T cells, with short telomeres and inactive telomerase, are different from exhausted cells, and may form due to defective telomere transfer reactions upon contact with antigen presenting cells (APCs). Senescent T cells are characterized by presence of sestrin-MAPK kinase activation complexes (sMACs), large immune-inhibitory protein assemblies of sestrins bound to a stress/energy sensing kinase (AMPK) and three functional effector kinases (ERK, JNK and p38 MAPKs). Here we described first in class Disruptors of the Sestrin-MAPK immune-inhibitory Complex (DOS), which target sMAC to ubiquitin-dependent proteasomal degradation, resulting in long-term sestrin transcriptional inhibition, increased T cell fitness, and generation of long-lived stem like memory features. Strikingly, the DOS generated stem T cells present de novo antigen-specific T-cell receptor DNA rearrangements that precede their future expansion. Although largely senescent at the point of treatment, the DOS regenerated T cells, with stem features and new TCRs, initiated immune-protective rejuvenation-dependent responses to new challenges, with or without vaccination. Therefore, it is possible to generate new T cell clones from formerly senescent cells and expand immune specificity. Highlights DOS are the first sestrin-MAPK binding disruptors DOS rejuvenate T cells (DOS-juvenation) DOS-juvenated T cells protect old mice from lethal infections, with or without vaccination DOS-juvenated T cells exist as stem-like cells that undergo antigen-specific TCR revisions

How to cite this publication

Alessio Lanna, Clara D’Ambra, Federica Rinaldi, Luisa Chocarro, Manuel Delpero, Melania Capitani, Michael Karin (2024). Disruptors of sestrin-MAPK interactions rejuvenate T cells and expand TCR specificity. , DOI: https://doi.org/10.1101/2024.05.17.594698.

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Publication Details

Type

Preprint

Year

2024

Authors

7

Datasets

0

Total Files

0

Language

en

DOI

https://doi.org/10.1101/2024.05.17.594698

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