Intratumoral CD103+CD8+ T cells predict response to neoadjuvant chemoimmunotherapy in advanced head and neck squamous cell carcinoma

Author:

Ren Siqi12,Lan Tianjun12,Wu Fan12,Chen Suling12,Jiang Xue2,Huo Chuying3,Li Zitian4,Xie Shule12,Wu Donghui5,Wang Ruixin12,Li Yanyan12,Qiu Lin12,Huang Guoxin12,Li Shurui2,Wang Xiaojuan2,Cen Meifeng2,Cai Tingting1,Lin Zhaoyu12,Li Jinsong12ORCID,Li Bowen12

Affiliation:

1. Department of Oral and Maxillofacial Surgery Sun Yat‐sen Memorial Hospital of Sun Yat‐sen University Guangdong P. R. China

2. Guangdong Provincial Key Laboratory of Malignant Tumor Epigenetics and Gene Regulation, Guangdong‐Hong Kong Joint Laboratory for RNA Medicine Medical Research Center, Sun Yat‐sen Memorial Hospital, Sun Yat‐sen University Guangdong P. R. China

3. Department of Gynecological Oncology Sun Yat‐sen Memorial Hospital, Sun Yat‐sen University Guangdong P. R. China

4. School of Stomatology, Jilin University Jilin P. R. China

5. Stomatology Hospital of Haizhu district Guangdong P. R. China

Abstract

AbstractBackgroundImmune cell heterogenicity is known to determine the therapeutic response to cancer progression. Neoadjuvant chemoimmunotherapy (NACI) has shown clinical benefits in some patients with advanced head and neck squamous cell carcinoma (HNSCC), but the underlying mechanism behind this clinical response is unknown. The efficacy of NACI needs to be potentiated by identifying accurate biomarkers to predict clinical responses. Here, we attempted to identify molecules predicting NACI response in advanced HNSCC.MethodsWe performed combined single‐cell RNA sequencing (scRNA‐seq) and multiplex immunofluorescence (mIHC) staining with tumor samples derived from NACI‐treated HNSCC patients to identify a new tumor‐infiltrating cell (TIL) subtype, CD103+CD8+ TILs, associated with clinical response, while both in vitro and in vivo assays were carried out to determine its antitumor efficiency. The regulatory mechanism of the CD103+CD8+ TILs population was examined by performing cell‐cell interaction analysis of the scRNA‐seq data and spatial analysis of the mIHC images.ResultsWe established intratumoral CD103+CD8+ TILs density as a determinant of NACI efficacy in cancers. Our scRNA‐seq results indicated that the population of CD103+CD8+ TILs was dramatically increased in the responders of NACI‐treated HNSCC patients, while mIHC analysis confirmed the correlation between intratumoral CD103+CD8+ TILs density and NACI efficacy in HNSCC patients. Further receiver operating characteristic curve analysis defined this TIL subset as a potent marker to predict patient response to NACI. Functional assays showed that CD103+CD8+ TILs were tumor‐reactive T cells, while programmed cell death protein‐1 (PD‐1) blockade enhanced CD103+CD8+ TILs cytotoxicity against tumor growth in vivo. Mechanistically, targeting the triggering receptor expressed on myeloid cells 2‐positive (TREM2+) macrophages might enhance the population of CD103+CD8+ TILs and facilitate antitumor immunity during NACI treatment.ConclusionsOur study highlights the impact of intratumoral CD103+CD8+ TILs density on NACI efficacy in different cancers, while the efforts to elevate its population warrant further clinical investigation.

Funder

China Postdoctoral Science Foundation

National Natural Science Foundation of China

Guangzhou Municipal Science and Technology Project

Publisher

Wiley

Subject

Cancer Research,Oncology

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