Extrachromosomal circular DNA orchestrates genome heterogeneity in urothelial bladder carcinoma

染色体外环状 DNA 调控膀胱尿路上皮癌的基因组异质性

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作者:Wei Lv, Xiaoguang Pan, Peng Han, Shuang Wu, Yuchen Zeng, Qingqing Wang, Lidong Guo, Mengyang Xu, Yanwei Qi, Li Deng, Zhe Xu, Conghui Li, Tianxi Yu, Xin Cui, Huajing Teng, Chongjun Xiang, Haotian Tan, Yue Li, Ning Liang, Huiying Tao, Qingqing Gao, Guohua Yu, Jia Mi, Fuyi Xu, Benjiao Gong, Lei Shi, Ta

Conclusions

Overall, our study provides a comprehensive extrachromosomal circular DNA map of UBC, along with valuable data resources and bioinformatics tools for future cancer and extrachromosomal circular DNA research.

Methods

We performed whole-genome/exome sequencing (WGS/WES), Circle-Seq, single-molecule real-time (SMRT) long-read sequencing of circular DNA, and RNA sequencing (RNA-Seq) on 80 pairs of tumor and AT samples. We used our newly developed circular DNA analysis software, Circle-Map++ to detect small extrachromosomal circular DNA from Circle-Seq data.

Results

We observed a high load and significant heterogeneity of extrachromosomal circular DNAs in UBC, including numerous single-locus and complex chimeric circular DNAs originating from different chromosomes. This includes highly chimeric circular DNAs carrying seven oncogenes and circles from nine chromosomes. We also found that large tumor-specific extrachromosomal circular DNAs could influence genome-wide gene expression, and are detectable in time-matched urinary sediments. Additionally, we found that the extrachromosomal circular DNA correlates with hypermutation, copy number variation, oncogene amplification, and clinical outcome. Conclusions: Overall, our study provides a comprehensive extrachromosomal circular DNA map of UBC, along with valuable data resources and bioinformatics tools for future cancer and extrachromosomal circular DNA research.

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