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The genetic landscape of high-risk neuroblastoma

ATRX公司 生物 神经母细胞瘤RAS病毒癌基因同源物 PTPN11型 神经母细胞瘤 种系突变 生殖系 外显子组测序 支票2 遗传学 体细胞 癌症研究 突变 外显子组 基因 克拉斯 细胞培养
作者
Trevor J. Pugh,Olena Morozova,Edward F. Attiyeh,Shahab Asgharzadeh,Jun S. Wei,Daniel Auclair,Scott L. Carter,Kristian Cibulskis,Megan Hanna,Adam Kieżun,Jaegil Kim,Michael S. Lawrence,Lee Lichenstein,Aaron McKenna,Chandra Sekhar Pedamallu,Alex H. Ramos,Erica Shefler,Andrey Sivachenko,Carrie Sougnez,Chip Stewart,Adrian Ally,İnanç Birol,Readman Chiu,Richard Corbett,Martin Hirst,Shaun Jackman,Baljit Kamoh,Alireza Hadj Khodabakshi,Martin Krzywinski,Allan Lo,Richard A. Moore,Karen Mungall,Jenny Q. Qian,Angela Tam,Nina Thiessen,Yongjun Zhao,Kristina A. Cole,Maura Diamond,Sharon J. Diskin,Yaël P. Mossé,Andrew Wood,Lingyun Ji,Richard Sposto,Thomas Badgett,Wendy B. London,Yvonne Moyer,Julie M. Gastier‐Foster,Malcolm A. Smith,Jaime M. Guidry Auvil,Daniela S. Gerhard,Michael D. Hogarty,Steven J.M. Jones,Sı́lvia Beà,Stacey Gabriel,Gad Getz,Robert C. Seeger,Javed Khan,Marco A. Marra,Matthew Meyerson,John M. Maris
出处
期刊:Nature Genetics [Nature Portfolio]
卷期号:45 (3): 279-284 被引量:1058
标识
DOI:10.1038/ng.2529
摘要

John Maris, Matthew Meyerson, Marco Marra and colleagues report results of a large-scale sequencing study of neuroblastoma. They observe a low median exonic mutation frequency and strikingly few recurrently mutated genes in these tumors, highlighting challenges for developing targeted therapeutic strategies based on frequently mutated oncogenic drivers. Neuroblastoma is a malignancy of the developing sympathetic nervous system that often presents with widespread metastatic disease, resulting in survival rates of less than 50%. To determine the spectrum of somatic mutation in high-risk neuroblastoma, we studied 240 affected individuals (cases) using a combination of whole-exome, genome and transcriptome sequencing as part of the Therapeutically Applicable Research to Generate Effective Treatments (TARGET) initiative. Here we report a low median exonic mutation frequency of 0.60 per Mb (0.48 nonsilent) and notably few recurrently mutated genes in these tumors. Genes with significant somatic mutation frequencies included ALK (9.2% of cases), PTPN11 (2.9%), ATRX (2.5%, and an additional 7.1% had focal deletions), MYCN (1.7%, causing a recurrent p.Pro44Leu alteration) and NRAS (0.83%). Rare, potentially pathogenic germline variants were significantly enriched in ALK, CHEK2, PINK1 and BARD1. The relative paucity of recurrent somatic mutations in neuroblastoma challenges current therapeutic strategies that rely on frequently altered oncogenic drivers.

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