Author
Listed:
- Guan-Tian Lang
(Fudan University Shanghai Cancer Center
Fudan University)
- Yi-Zhou Jiang
(Fudan University Shanghai Cancer Center)
- Jin-Xiu Shi
(Chinese National Human Genome Center at Shanghai (CHGC) and Shanghai Academy of Science and Technology (SAST))
- Fan Yang
(Fudan University Shanghai Cancer Center
Fudan University)
- Xiao-Guang Li
(Fudan University Shanghai Cancer Center)
- Yu-Chen Pei
(Fudan University Shanghai Cancer Center
Precision Cancer Medical Center Affiliated to Fudan University Shanghai Cancer Center)
- Chen-Hui Zhang
(Chinese National Human Genome Center at Shanghai (CHGC) and Shanghai Academy of Science and Technology (SAST))
- Ding Ma
(Fudan University Shanghai Cancer Center)
- Yi Xiao
(Fudan University Shanghai Cancer Center)
- Peng-Chen Hu
(Chinese National Human Genome Center at Shanghai (CHGC) and Shanghai Academy of Science and Technology (SAST))
- Hai Wang
(Fudan University Shanghai Cancer Center
Fudan University)
- Yun-Song Yang
(Fudan University Shanghai Cancer Center
Fudan University)
- Lin-Wei Guo
(Fudan University Shanghai Cancer Center
Fudan University)
- Xun-Xi Lu
(Fudan University Shanghai Cancer Center
Fudan University)
- Meng-Zhu Xue
(Chinese Academy of Sciences)
- Peng Wang
(Chinese Academy of Sciences)
- A-Yong Cao
(Fudan University Shanghai Cancer Center)
- Hong Ling
(Fudan University Shanghai Cancer Center)
- Zhong-Hua Wang
(Fudan University Shanghai Cancer Center)
- Ke-Da Yu
(Fudan University Shanghai Cancer Center)
- Gen-Hong Di
(Fudan University Shanghai Cancer Center)
- Da-Qiang Li
(Fudan University Shanghai Cancer Center)
- Yun-Jin Wang
(Fudan University Shanghai Cancer Center
Precision Cancer Medical Center Affiliated to Fudan University Shanghai Cancer Center)
- Ying Yu
(Fudan University)
- Le-Ming Shi
(Fudan University)
- Xin Hu
(Fudan University Shanghai Cancer Center
Precision Cancer Medical Center Affiliated to Fudan University Shanghai Cancer Center)
- Wei Huang
(Chinese National Human Genome Center at Shanghai (CHGC) and Shanghai Academy of Science and Technology (SAST)
Precision Cancer Medical Center Affiliated to Fudan University Shanghai Cancer Center)
- Zhi-Ming Shao
(Fudan University Shanghai Cancer Center
Precision Cancer Medical Center Affiliated to Fudan University Shanghai Cancer Center)
Abstract
The remarkable advances in next-generation sequencing technology have enabled the wide usage of sequencing as a clinical tool. To promote the advance of precision oncology for breast cancer in China, here we report a large-scale prospective clinical sequencing program using the Fudan-BC panel, and comprehensively analyze the clinical and genomic characteristics of Chinese breast cancer. The mutational landscape of 1,134 breast cancers reveals that the most significant differences between Chinese and Western patients occurred in the hormone receptor positive, human epidermal growth factor receptor 2 negative breast cancer subtype. Mutations in p53 and Hippo signaling pathways are more prevalent, and 2 mutually exclusive and 9 co-occurring patterns exist among 9 oncogenic pathways in our cohort. Further preclinical investigation partially suggests that NF2 loss-of-function mutations can be sensitive to a Hippo-targeted strategy. We establish a public database (Fudan Portal) and a precision medicine knowledge base for data exchange and interpretation. Collectively, our study presents a leading approach to Chinese precision oncology treatment and reveals potentially actionable mutations in breast cancer.
Suggested Citation
Guan-Tian Lang & Yi-Zhou Jiang & Jin-Xiu Shi & Fan Yang & Xiao-Guang Li & Yu-Chen Pei & Chen-Hui Zhang & Ding Ma & Yi Xiao & Peng-Chen Hu & Hai Wang & Yun-Song Yang & Lin-Wei Guo & Xun-Xi Lu & Meng-Zh, 2020.
"Characterization of the genomic landscape and actionable mutations in Chinese breast cancers by clinical sequencing,"
Nature Communications, Nature, vol. 11(1), pages 1-13, December.
Handle:
RePEc:nat:natcom:v:11:y:2020:i:1:d:10.1038_s41467-020-19342-3
DOI: 10.1038/s41467-020-19342-3
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