Flt3L-mediated tumor cDC1 expansion enhances immunotherapy by priming stem-like CD8 T cells in lymph nodes

J Lai; CW Chan; JD Armitage; KM Audsley; YK Huang; EB Derrick; LS Carstensen; CM Scheffler; ME Jones; K Sek; N Principe; JS Kim; IG House; AXY Chen; KM Yap; J Middelburg; I Munoz; D Nguyen; J Tong; TX Hoang; KL Todd; M Evrard; J Chee; LK Mackay; ARR Forrest; IA Parish; A Bosco; J Waithman; PA Beavis; PK Darcy

Journal article

Flt3L-mediated tumor cDC1 expansion enhances immunotherapy by priming stem-like CD8 T cells in lymph nodes

J Lai, CW Chan, JD Armitage, KM Audsley, YK Huang, EB Derrick, LS Carstensen, CM Scheffler, ME Jones, K Sek, N Principe, JS Kim, IG House, AXY Chen, KM Yap, J Middelburg, I Munoz, D Nguyen, J Tong, TX Hoang Show all

Nature Immunology | Published : 2026

DOI: 10.1038/s41590-026-02419-4

Abstract

Immune checkpoint blockade (ICB) evokes antitumor immunity through the reinvigoration of T cell responses. T cell differentiation status controls response, with less differentiated cells having an enhanced capacity to proliferate after ICB. Given that conventional type 1 dendritic cells (cDC1) maintain precursor exhausted T cells (TPEX), we hypothesized that expansion of cDC1s with Flt3L could enhance responses to ICB. Here we show that treatment with Fms-related tyrosine kinase 3 ligand (Flt3L) expands CD62L+SLAMF6+CD8+ T cells in the tumor through a mechanism that requires XCR1+ dendritic cells to traffic to the tumor-draining lymph node. The combination of Flt3L and anti-CTLA-4 enhanced t..

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