Single-cell transcriptomics reveals cell atlas and identifies cycling tumor cells responsible for recurrence in ameloblastoma.
Gan XiongNan XieMin NieRongsong LingBokai YunJiaxiang XieLinlin RenYaqi HuangWenjin WangChen YiMing ZhangXiuyun XuCaihua ZhangBin ZouLeitao ZhangXiqiang LiuHongzhang HuangDemeng ChenWei CaoCheng WangPublished in: International journal of oral science (2024)
Ameloblastoma is a benign tumor characterized by locally invasive phenotypes, leading to facial bone destruction and a high recurrence rate. However, the mechanisms governing tumor initiation and recurrence are poorly understood. Here, we uncovered cellular landscapes and mechanisms that underlie tumor recurrence in ameloblastoma at single-cell resolution. Our results revealed that ameloblastoma exhibits five tumor subpopulations varying with respect to immune response (IR), bone remodeling (BR), tooth development (TD), epithelial development (ED), and cell cycle (CC) signatures. Of note, we found that CC ameloblastoma cells were endowed with stemness and contributed to tumor recurrence, which was dominated by the EZH2-mediated program. Targeting EZH2 effectively eliminated CC ameloblastoma cells and inhibited tumor growth in ameloblastoma patient-derived organoids. These data described the tumor subpopulation and clarified the identity, function, and regulatory mechanism of CC ameloblastoma cells, providing a potential therapeutic target for ameloblastoma.
Keyphrases
- single cell
- induced apoptosis
- cell cycle
- rna seq
- immune response
- emergency department
- cell cycle arrest
- stem cells
- cell proliferation
- high throughput
- machine learning
- genome wide
- long non coding rna
- bone marrow
- transcription factor
- electronic health record
- signaling pathway
- inflammatory response
- artificial intelligence
- endoplasmic reticulum stress
- high intensity
- mesenchymal stem cells
- deep learning
- single molecule