Abstract

High functional heterogeneity of cancer cells poses a major challenge for cancer research. Single-cell sequencing technology provides an unprecedented opportunity to decipher diverse functional states of cancer cells at single-cell resolution, and cancer scRNA-seq datasets have been largely accumulated. This emphasizes the urgent need to build a dedicated resource to decode the functional states of cancer single cells. Here, we developed CancerSEA (http://biocc.hrbmu.edu.cn/CancerSEA/ or http://202.97.205.69/CancerSEA/), the first dedicated database that aims to comprehensively explore distinct functional states of cancer cells at the single-cell level. CancerSEA portrays a cancer single-cell functional state atlas, involving 14 functional states (including stemness, invasion, metastasis, proliferation, EMT, angiogenesis, apoptosis, cell cycle, differentiation, DNA damage, DNA repair, hypoxia, inflammation and quiescence) of 41 900 cancer single cells from 25 cancer types. It allows querying which functional states are associated with the gene (or gene list) of interest in different cancers. CancerSEA also provides functional state-associated PCG/lncRNA repertoires across all cancers, in specific cancers, and in individual cancer single-cell datasets. In summary, CancerSEA provides a user-friendly interface for comprehensively searching, browsing, visualizing and downloading functional state activity profiles of tens of thousands of cancer single cells and the corresponding PCGs/lncRNAs expression profiles.

Keywords

BiologyCancerCancer cellComputational biologySingle-cell analysisCellMetastasisDNA repairCancer stem cellCell cycleCancer researchGeneticsBioinformaticsGene

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Publication Info

Year
2018
Type
article
Volume
47
Issue
D1
Pages
D900-D908
Citations
1045
Access
Closed

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Huating Yuan, Min Yan, Guanxiong Zhang et al. (2018). CancerSEA: a cancer single-cell state atlas. Nucleic Acids Research , 47 (D1) , D900-D908. https://doi.org/10.1093/nar/gky939

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DOI
10.1093/nar/gky939