Single cell multi-omics reveal intra-cell-line heterogeneity across human cancer cell lines.
Qionghua ZhuXin ZhaoYuanhang ZhangYanping LiShang LiuJingxuan HanZhiyuan SunChunqing WangDaqi DengShanshan WangYisen TangYaling HuangSiyuan JiangChi TianXi ChenYue YuanZeyu LiTao YangTingting LaiYiqun LiuWenzhen YangXuanxuan ZouMingyuan ZhangHuanhuan CuiChuanyu LiuXin JinYuhui HuAo ChenXue LiuGuipeng LiYong HouLongqi LiuShi-Ping LiuLiang FangWei ChenLiang WuPublished in: Nature communications (2023)
Human cancer cell lines have long served as tools for cancer research and drug discovery, but the presence and the source of intra-cell-line heterogeneity remain elusive. Here, we perform single-cell RNA-sequencing and ATAC-sequencing on 42 and 39 human cell lines, respectively, to illustrate both transcriptomic and epigenetic heterogeneity within individual cell lines. Our data reveal that transcriptomic heterogeneity is frequently observed in cancer cell lines of different tissue origins, often driven by multiple common transcriptional programs. Copy number variation, as well as epigenetic variation and extrachromosomal DNA distribution all contribute to the detected intra-cell-line heterogeneity. Using hypoxia treatment as an example, we demonstrate that transcriptomic heterogeneity could be reshaped by environmental stress. Overall, our study performs single-cell multi-omics of commonly used human cancer cell lines and offers mechanistic insights into the intra-cell-line heterogeneity and its dynamics, which would serve as an important resource for future cancer cell line-based studies.
Keyphrases
- single cell
- rna seq
- papillary thyroid
- high throughput
- endothelial cells
- squamous cell
- copy number
- gene expression
- dna methylation
- induced pluripotent stem cells
- genome wide
- lymph node metastasis
- squamous cell carcinoma
- public health
- drug discovery
- childhood cancer
- young adults
- circulating tumor
- climate change
- oxidative stress
- heat stress
- human health
- cell free