Genomic landscape and genetic heterogeneity in gastric adenocarcinoma revealed by whole-genome sequencing

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作者
Swee Seong Wong
Kyoung-Mee Kim
Jason C. Ting
Kun Yu
Jake Fu
Shawn Liu
Razvan Cristescu
Michael Nebozhyn
Lara Gong
Yong Gang Yue
Jian Wang
Chen Ronghua
Andrey Loboda
James Hardwick
Xiaoqiao Liu
Hongyue Dai
Jason Gang Jin
Xiang S. Ye
So Young Kang
In Gu Do
Joon Oh Park
Tae Sung Sohn
Christoph Reinhard
Jeeyun Lee
Sung Kim
Amit Aggarwal
机构
[1] Lilly Research Labs,Department of Pathology & Translational Genomics
[2] Eli Lilly and Co,Division of Hematology
[3] Samsung Medical Center,Oncology, Department of Medicine
[4] Sungkyunkwan University School of Medicine,Department of Surgery
[5] Shanghai Biocorp,undefined
[6] BGI Techsolutions,undefined
[7] Merck Research Labs,undefined
[8] Merck Sharpe & Dohme,undefined
[9] Samsung Medical Center,undefined
[10] Sungkyunkwan University School of Medicine,undefined
[11] Samsung Medical Center,undefined
[12] Sungkyunkwan University School of Medicine,undefined
[13] Present address: Novartis Institute for Biomedical Research,undefined
[14] Boston,undefined
[15] Massachusetts,undefined
[16] USA,undefined
[17] Present address: Pfizer,undefined
[18] San Diego,undefined
[19] California,undefined
[20] USA,undefined
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摘要
Gastric cancer (GC) is the second most common cause of cancer-related deaths. It is known to be a heterogeneous disease with several molecular and histological subtypes. Here we perform whole-genome sequencing of 49 GCs with diffuse (N=31) and intestinal (N=18) histological subtypes and identify three mutational signatures, impacting TpT, CpG and TpCp[A/T] nucleotides. The diffuse-type GCs show significantly lower clonality and smaller numbers of somatic and structural variants compared with intestinal subtype. We further divide the diffuse subtype into one with infrequent genetic changes/low clonality and another with relatively higher clonality and mutations impacting TpT dinucleotide. Notably, we discover frequent and exclusive mutations in Ephrins and SLIT/ROBO signalling pathway genes. Overall, this study delivers new insights into the mutational heterogeneity underlying distinct histologic subtypes of GC that could have important implications for future research in the diagnosis and treatment of GC.
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