Single-cell transcriptome analysis of epithelial, immune, and stromal signatures and interactions in human ovarian cancer

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作者
Chaochao Chai
Langchao Liang
Nanna S. Mikkelsen
Wei Wang
Wandong Zhao
Chengcheng Sun
Rasmus O. Bak
Hanbo Li
Lin Lin
Fei Wang
Yonglun Luo
机构
[1] University of Chinese Academy of Sciences,College of Life Sciences
[2] Lars Bolund Institute of Regenerative Medicine Qingdao-Europe Advanced Institute for LifeScience,Department of Biomedicine
[3] BGI Research,Department of Obstetrics and Gynecology, Tongji Hospital, Tongji Medical College
[4] BGI Research,Steno Diabetes Center Aarhus
[5] Aarhus University,undefined
[6] Huazhong University of Science and Technology,undefined
[7] Aarhus University Hospital,undefined
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A comprehensive investigation of ovarian cancer (OC) progression at the single-cell level is crucial for enhancing our understanding of the disease, as well as for the development of better diagnoses and treatments. Here, over half a million single-cell transcriptome data were collected from 84 OC patients across all clinical stages. Through integrative analysis, we identified heterogeneous epithelial-immune-stromal cellular compartments and their interactions in the OC microenvironment. The epithelial cells displayed clinical subtype features with functional variance. A significant increase in distinct T cell subtypes was identified including Tregs and CD8+ exhausted T cells from stage IC2. Additionally, we discovered antigen-presenting cancer-associated fibroblasts (CAFs), with myofibroblastic CAFs (myCAFs) exhibiting enriched extracellular matrix (ECM) functionality linked to tumor progression at stage IC2. Furthermore, the NECTIN2-TIGIT ligand-receptor pair was identified to mediate T cells communicating with epithelial, fibroblast, endothelial, and other cell types. Knock-out of NECTIN2 using CRISPR/Cas9 inhibited ovarian cancer cell (SKOV3) proliferation, and increased T cell proliferation when co-cultured. These findings shed light on the cellular compartments and functional aspects of OC, providing insights into the molecular mechanisms underlying stage IC2 and potential therapeutic strategies for OC.
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