Single cell analysis in head and neck cancer reveals potential immune evasion mechanisms during early metastasis

头颈癌单细胞分析揭示早期转移过程中潜在的免疫逃逸机制

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作者:Hong Sheng Quah # ,Elaine Yiqun Cao # ,Lisda Suteja ,Constance H Li ,Hui Sun Leong ,Fui Teen Chong ,Shilpi Gupta ,Camille Arcinas ,John F Ouyang ,Vivian Ang ,Teja Celhar ,Yunqian Zhao ,Hui Chen Tay ,Jerry Chan ,Takeshi Takahashi ,Daniel S W Tan ,Subhra K Biswas ,Owen J L Rackham ,N Gopalakrishna Iyer

Abstract

Profiling tumors at single-cell resolution provides an opportunity to understand complexities underpinning lymph-node metastases in head and neck squamous-cell carcinoma. Single-cell RNAseq (scRNAseq) analysis of cancer-cell trajectories identifies a subpopulation of pre-metastatic cells, driven by actionable pathways including AXL and AURK. Blocking these two proteins blunts tumor invasion in patient-derived cultures. Furthermore, scRNAseq analyses of tumor-infiltrating CD8 + T-lymphocytes show two distinct trajectories to T-cell dysfunction, corroborated by their clonal architecture based on single-cell T-cell receptor sequencing. By determining key modulators of these trajectories, followed by validation using external datasets and functional experiments, we uncover a role for SOX4 in mediating T-cell exhaustion. Finally, interactome analyses between pre-metastatic tumor cells and CD8 + T-lymphocytes uncover a putative role for the Midkine pathway in immune-modulation and this is confirmed by scRNAseq of tumors from humanized mice. Aside from specific findings, this study demonstrates the importance of tumor heterogeneity analyses in identifying key vulnerabilities during early metastasis.

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