PO.CL05.01 · 临床研究
Sentinel lymph node-derived CD45⁺ cells combined with low-dose radiotherapy and PD-1 blockade as a next-generation adoptive cell therapy in head and neck cancer
作者与单位
摘要 Abstract
Purpose: Head and neck squamous cell carcinoma (HNSCC) is the seventh most common cancer globally, representing roughly 6% of all malignancies. Each year it accounts for an estimated 660,000 new diagnoses and over 325,000 deaths, with incidence projected to rise by nearly 30% by 2030. Despite advances in surgery, radiation, and immunotherapy, patients with HPV-negative HNSCC continue to face poor outcomes, with five-year overall survival rates often below 55%. Adoptive cell therapy (ACT) in solid tumors remains limited by the scarcity of tumor-reactive T cells and their functional exhaustion after expansion. The sentinel lymph node (SLN), the initial site of tumor antigen presentation and T-cell priming, may provide a rich and minimally exhausted source of tumor-specific lymphocytes. Here, we evaluated the immunologic and therapeutic advantages of SLN-derived leukocytes over those from tumor tissue in an orthotopic model of HPV⁻ HNSCC.
Methods: CD45⁺ immune cells isolated from donor SLNs, NSLNs, tumors, or SLNs preconditioned with low-dose tdRT (4 Gy) in the 4MOSC1 murine model were adoptively transferred into syngeneic tumor-bearing recipients to evaluate their therapeutic potential. Recipient groups included untreated controls, preconditioned mice with 4 Gy tdRT, or a single PD-1 blockade (PD1i) dose before ACT. Phenotypic and functional characterization was performed using flow cytometry, multiplex immunofluorescence, ELISA, and CITE-seq to evaluate cell populations, activation, exhaustion, clonal overlap, and tissue distribution.
Results: SLN-CD45⁺ populations were enriched in activated CD4⁺/CD8⁺ T cells with elevated CD69, CD137, and IFN-gamma expression compared with tumor-derived counterparts. mIHC confirmed higher densities of activated T cells in SLN and tumor regions after SLN-CD45⁺ transfer. TCR analysis revealed substantial overlap between SLN and tumor clonotypes, suggesting selective enrichment of tumor-reactive clones. Functionally, ACT with SLN-CD45⁺ cells induced greater tumor regression and survival benefits than ACT from tumor source, even without lymphodepletion or expansion in culture. Notably, cryopreserved SLN-derived cells retained comparable efficacy to freshly isolated ones. Preconditioning recipients with 4 Gy tdRT or PD1i further improved intratumoral infiltration, activation, and persistence of transferred cells without added toxicity.
Conclusions: The sentinel lymph node provides a potent, readily accessible reservoir of tumor-reactive immune cells for ACT. Combining SLN-derived ACT with tdRT and PD1i significantly enhances therapeutic efficacy in HPV⁻ HNSCC. These findings highlight the translational potential of leveraging tumor-draining lymphoid niches as tumor-primed immune reservoirs for next-generation ACT in solid tumors.
利益披露 Disclosure
P. Mohammadzadeh, None..
T. Kurokawa, None..
K. Decker, None..
P. Vo, None..
P. Sen, None..
R. Jones, None..
S. Miyauchi, None..
S. Fassardi, None..
A. Zourelidis, None..
R. Saddawi-Konefka, None..
J. Califano, None.