PO.IM01.04 · 免疫学
Paclitaxel induces colocalization of CXCL9⁺ tumor-associated macrophages and CD8⁺ T cells to potentiate antitumor immunity in head and neck squamous cell carcinoma
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摘要 Abstract
Background: Paclitaxel is a key chemotherapeutic agent for head and neck squamous cell carcinoma (HNSCC). Recent studies have suggested the role of paclitaxel in immune responses, particularly relevant to tumor-associated macrophages (TAMs). This study explores the immunomodulatory role of paclitaxel in the tumor microenvironment (TME), focusing on its interaction with TAMs in HNSCC.
Methods: In vitro and in vivo studies were conducted on murine samples and human samples from our tertiary referral center. The in vitro experiment involved murine bone marrow-derived macrophages (BMDMs) to evaluate phagocytic functions and the expression of MHC-related genes and proteins. Our in vivo study aimed to discriminate the spatial characteristics of SPP1+/CXCL9+ TAMs and their interaction with CD8+ T cells, especially under exposure to paclitaxel, using mouse oral carcinoma (MOC) and HNSCC samples.
Results: Paclitaxel enhanced macrophage phagocytosis and upregulated antigen processing genes. In the murine HNSCC model, paclitaxel combined with anti-PD-1 significantly suppressed tumor growth, whereas either treatment alone was ineffective. This was associated with the redistribution of CXCL9+ TAMs into the tumor core. Consistently, human HNSCC samples demonstrated that paclitaxel-based neoadjuvant chemotherapy (NAC) was linked to improved survival and increased infiltration of CXCL9+ TAMs and CD8+ T cells into the tumor core, indicating a shift from an "immune-excluded" to an "inflamed" microenvironment.
Conclusion: Paclitaxel upregulates the phagocytic and antigen-presenting function of TAMs while spatially redistributing them toward the tumor core and subsequently inducing CD8+ T cell infiltration. Such features suggest that Paclitaxel may reprogram an immune-deserted TME to an anti-tumoral condition, ultimately contributing to immunotherapy responsiveness.
利益披露 Disclosure
M. Kwon, None..
J. Kim, None..
J. Hong, None..
S. Choi, None..
J. Kim, None..
H. Cho, None..
M. Park, None..
J. Seo, None..
J. Park, None.