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Germline pathogenic variants in neuroblastoma patients are enriched in BARD1 and predict worse survival

生殖系 优势比 种系突变 神经母细胞瘤 生物 内科学 癌症 基因型 遗传学 医学 突变 基因 细胞培养
作者
Jung Kim,Zalman Vaksman,Laura E. Egolf,Rebecca Kaufman,Perry Evans,Karina L. Conkrite,Arnavaz Danesh,Gonzalo López,Michael P. Randall,Maiah H. Dent,Lance M. Farra,Neil Menghani,Malwina Dymek,Heena Desai,Ryan Hausler,Belynda Hicks,Jaime Guidry Auvil,Daniela S. Gerhard,Hákon Hákonarson,Kara N. Maxwell,Kristina A. Cole,Trevor J. Pugh,Kristopher R. Bosse,Javed Khan,Jun S. Wei,John M. Maris,Douglas R. Stewart,Sharon J. Diskin
出处
期刊:Journal of the National Cancer Institute [Oxford University Press]
卷期号:116 (1): 149-159 被引量:5
标识
DOI:10.1093/jnci/djad183
摘要

Abstract Background Neuroblastoma is an embryonal cancer of the developing sympathetic nervous system. The genetic contribution of rare pathogenic or likely pathogenic germline variants in patients without a family history remains unclear. Methods Germline DNA sequencing was performed on 786 neuroblastoma patients. The frequency of rare cancer predisposition gene pathogenic or likely pathogenic variants in patients was compared with 2 cancer-free control cohorts. Matched tumor DNA sequencing was evaluated for second hits, and germline DNA array data from 5585 neuroblastoma patients and 23 505 cancer-free control children were analyzed to identify rare germline copy number variants. Patients with germline pathogenic or likely pathogenic variants were compared with those without to test for association with clinical characteristics, tumor features, and survival. Results We observed 116 pathogenic or likely pathogenic variants involving 13.9% (109 of 786) of neuroblastoma patients, representing a statistically significant excess burden compared with cancer-free participants (odds ratio [OR] = 1.60, 95% confidence interval [CI] = 1.27 to 2.00). BARD1 harbored the most statistically significant enrichment of pathogenic or likely pathogenic variants (OR = 32.30, 95% CI = 6.44 to 310.35). Rare germline copy number variants disrupting BARD1 were identified in patients but absent in cancer-free participants (OR = 29.47, 95% CI = 1.52 to 570.70). Patients harboring a germline pathogenic or likely pathogenic variant had a worse overall survival compared with those without (P = 8.6 x 10−3). Conclusions BARD1 is an important neuroblastoma predisposition gene harboring both common and rare germline pathogenic or likely pathogenic variations. The presence of any germline pathogenic or likely pathogenic variant in a cancer predisposition gene was independently predictive of worse overall survival. As centers move toward paired tumor-normal sequencing at diagnosis, efforts should be made to centralize data and provide an infrastructure to support cooperative longitudinal prospective studies of germline pathogenic variation.

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