Enhanced ICOS Signaling Between Dendritic Cells and T Cells Characterizes the Immune Landscape of Human Cholangiocarcinoma
Meiying Zhu, Yuou Li, Xiaolong Tang, Xinjian Wan, Zunqiang Zhou

TL;DR
This study identifies enhanced ICOS signaling between dendritic cells and T cells in cholangiocarcinoma, suggesting a new target for immunotherapy.
Contribution
The study reveals a novel role of ICOS signaling in tumor-immune interactions in cholangiocarcinoma.
Findings
Tumor-associated dendritic cells, especially plasmacytoid DCs, show increased ICOS-mediated communication with T cells.
Tumor-conditioned dendritic cells upregulate ICOSL and activate CD8+ T cells through the ICOS–ICOSL axis.
Blocking ICOSL abolishes T-cell activation, confirming the functional importance of this signaling pathway.
Abstract
Cholangiocarcinoma exhibits a complex tumor microenvironment, yet the cellular interactions governing its progression remain poorly understood. Here, through integrated analysis of two independent single-cell RNA sequencing datasets comprising both complete tissue and immune-focused profiling, we comprehensively mapped the cellular landscape and intercellular communication networks in human cholangiocarcinoma. Our analysis revealed significant remodeling of immune cell compositions and interaction patterns in the tumor microenvironment. Notably, we identified enhanced ICOS signaling between dendritic cells and T cells as a prominent feature of cholangiocarcinoma. Using CellChat analysis, we demonstrated that tumor-associated dendritic cells, particularly plasmacytoid DCs, exhibit stronger ICOS-mediated communication with T cells compared to their counterparts in normal tissues.…
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Taxonomy
TopicsCholangiocarcinoma and Gallbladder Cancer Studies · MicroRNA in disease regulation · Cancer Mechanisms and Therapy
