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. 2025 Oct;26(10):1752-1765.
doi: 10.1038/s41590-025-02276-7. Epub 2025 Sep 15.

Lymph nodes fuel KLF2-dependent effector CD8+ T cell differentiation during chronic infection and checkpoint blockade

Carlson Tsui #  1 Leonie Heyden #  2   3 Lifen Wen  2 Catarina Gago da Graça  2 Nikita Potemkin  2 Aleksej Frolov  2   4 Daniel Rawlinson  2 Lei Qin  2 Verena C Wimmer  5 Marjan Hadian-Jazi  5   6 Darya Malko  2   4 Chun-Hsi Su  2 Sining Li  2 Kayla R Wilson  2 Helena Horvatic  2   3 Sharanya K Wijesinghe  2 Marcela L Moreira  2 Lachlan Dryburgh  2 Dominik Schienstock  2 Lisa Rausch  2 Daniel T Utzschneider  2 Cornelia Halin  7 Scott N Mueller  2 Marc D Beyer  4   8   9 Sammy Bedoui  2 Zeinab Abdullah  3 Jan Schröder  2 Axel Kallies  10   11
Affiliations

Lymph nodes fuel KLF2-dependent effector CD8+ T cell differentiation during chronic infection and checkpoint blockade

Carlson Tsui et al. Nat Immunol. 2025 Oct.

Abstract

Exhausted CD8+ T (TEX) cell responses are maintained by precursors of exhausted T (TPEX) cells that possess high self-renewal and developmental potential. TPEX cells also drive the proliferative burst of effector T cells upon therapeutic immune checkpoint blockade (ICB). However, the spatial context and signals that regulate their differentiation and function are not well defined. Here we identify developmental and functional compartmentalization of TPEX and TEX cells across secondary lymphoid organs during chronic infection. We show that stem-like CD62L+ TPEX and effector-like CX3CR1+ TEX cells constitute a distinct developmental lineage that is promoted by the lymph node (LN) microenvironment and dependent on the transcription factor KLF2. LNs act as a niche in which migratory dendritic cells provide antigen and costimulatory signals to maintain the proliferative fitness of CD62L+ TPEX cells and generation of CX3CR1+ TEX cells. Moreover, LNs exclusively drive the proliferative burst and systemic dissemination of CX3CR1+ TEX cells during ICB. Thus, our findings identify a unique role for LNs in the maintenance of T cell differentiation and function during systemic chronic infection and ICB therapy.

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Conflict of interest statement

Competing interests: A.K. has received research support from Pfizer. The other authors declare no competing interests.

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