Lymphatic egress recycles tumor-experienced effector CD8 T cells to sustain immune surveillance

Ines Delclaux
Katherine S. Ventre
Naomi R. Besson
Tara Muijlwijk
Milad Ibrahim
Guanning Wang
Taylor A. Heim
Maria M. Steele
Alexander C. Huang
Markus Schober
Iman Osman
Amanda W. Lund

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Abstract

Successful anti-tumor immune surveillance depends on stem-like CD8 ⁺ T cells that are enriched in tumor-draining lymph nodes (LN), but how they are maintained over time remains poorly understood. Here, we identify a continuous lymphatic circuit that sustains stem-like CD8 ⁺ T cells. Using photoconversion to fate-map intratumoral T cells we demonstrate that effector cells exit the tumor microenvironment and migrate back to the draining LN. These tumor-specific, migratory effector T cells avoid chronic antigen stimulation, re-express the transcription factor associated with self-renewal, TCF1, and enter a stem-like state in the LN. Antigen presentation in LNs by dendritic cells drives their proliferation thereby inflating the LN stem-like population. Consequently, maintenance of stem-like T cells and ICB response depends on constitutive lymphatic transport, while LN metastasis compromises the stem-like niche, diminishing ICB response. We, therefore, define a continuous, peripheral lymphatic circuit that recycles tumor-experienced effector T cells to fuel durable, systemic immune surveillance.

Version published to 10.64898/2026.04.30.721705 on bioRxiv
May 5, 2026

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