Intra-Tumor Genetic Heterogeneity in Wilms Tumor: Clonal Evolution and Clinical Implications

被引:62
|
作者
Cresswell, George D. [1 ]
Apps, John R. [2 ,3 ]
Chagtai, Tasnim [2 ]
Mifsud, Borbala [1 ]
Bentley, Christopher C. [1 ,4 ]
Maschietto, Mariana [2 ]
Popov, Sergey D. [5 ,6 ]
Weeks, Mark E. [2 ]
Olsen, Oystein E. [7 ]
Sebire, Neil J. [2 ,8 ]
Pritchard-Jones, Kathy [2 ,3 ]
Luscombe, Nicholas M. [1 ,4 ,9 ]
Williams, Richard D. [2 ]
Mifsud, William [2 ,8 ]
机构
[1] Francis Crick Inst, London, England
[2] UCL Inst Child Hlth, London, England
[3] Great Ormond St Hosp Sick Children, Dept Paediat Haematol & Oncol, London, England
[4] UCL, Dept Genet Evolut & Environm, UCL Genet Inst, London, England
[5] Inst Canc Res, Div Mol Pathol, London, England
[6] Inst Canc Res, Div Canc Therapeut, London, England
[7] Great Ormond St Hosp Sick Children, Dept Radiol, London, England
[8] Great Ormond St Hosp Sick Children, Dept Histopathol, London, England
[9] Okinawa Inst Sci & Technol, Okinawa, Japan
来源
EBIOMEDICINE | 2016年 / 9卷
基金
欧盟第七框架计划;
关键词
Intra-tumor genetic heterogeneity; Pediatric solid tumors; Wilms tumor; Tumor evolution; Tumor multisampling; Molecular biomarkers; Copy number aberrations; 11P15; ABNORMALITIES; H19; LOCUS; CANCER; MUTATIONS; EVENT; RISK; CHILDHOOD; DIVERSITY; RELAPSE; GAIN;
D O I
10.1016/j.ebiom.2016.05.029
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
The evolution of pediatric solid tumors is poorly understood. There is conflicting evidence of intra-tumor genetic homogeneity vs. heterogeneity (ITGH) in a small number of studies in pediatric solid tumors. A number of copy number aberrations (CNA) are proposed as prognostic biomarkers to stratify patients, for example 1q+ in Wilms tumor (WT); current clinical trials use only one sample per tumor to profile this genetic biomarker. We multisampled 20 WT cases and assessed genome-wide allele-specific CNA and loss of heterozygosity, and inferred tumor evolution, using Illumina CytoSNP12v2.1 arrays, a custom analysis pipeline, and the MEDICC algorithm. We found remarkable diversity of ITGH and evolutionary trajectories inWT. 1q+ is heterogeneous in the majority of tumors with this change, with variable evolutionary timing. We estimate that at least three samples per tumor are needed to detect >95% of cases with 1q+. In contrast, somatic 11p15 LOH is uniformly an early event inWT development. We find evidence of two separate tumor origins in unilateral disease with divergent histology, and in bilateral WT. We also show subclonal changes related to differential response to chemotherapy. Rational trial design to include biomarkers in risk stratification requires tumor multisampling and reliable delineation of ITGH and tumor evolution. (C) 2016 The Authors. Published by Elsevier B.V.
引用
收藏
页码:120 / 129
页数:10
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