Genomic profile of MYCN non-amplified neuroblastoma and potential for immunotherapeutic strategies in neuroblastoma

Eunjin Lee; Ji Won Lee; Boram Lee; Kyunghee Park; Joonho Shim; Keon Hee Yoo; Hong Hoe Koo; Ki Woong Sung; Woong-Yang Park

doi:10.1186/s12920-020-00819-5

BMC Medical Genomics (Nov 2020)

Genomic profile of MYCN non-amplified neuroblastoma and potential for immunotherapeutic strategies in neuroblastoma

Eunjin Lee,
Ji Won Lee,
Boram Lee,
Kyunghee Park,
Joonho Shim,
Keon Hee Yoo,
Hong Hoe Koo,
Ki Woong Sung,
Woong-Yang Park

Affiliations

Eunjin Lee: Samsung Genome Institute, Samsung Medical Center
Ji Won Lee: Department of Pediatrics, Samsung Medical Center, Sungkyunkwan University School of Medicine
Boram Lee: Samsung Genome Institute, Samsung Medical Center
Kyunghee Park: Samsung Genome Institute, Samsung Medical Center
Joonho Shim: Samsung Genome Institute, Samsung Medical Center
Keon Hee Yoo: Department of Pediatrics, Samsung Medical Center, Sungkyunkwan University School of Medicine
Hong Hoe Koo: Department of Pediatrics, Samsung Medical Center, Sungkyunkwan University School of Medicine
Ki Woong Sung: Department of Pediatrics, Samsung Medical Center, Sungkyunkwan University School of Medicine
Woong-Yang Park: Samsung Genome Institute, Samsung Medical Center

DOI: https://doi.org/10.1186/s12920-020-00819-5
Journal volume & issue: Vol. 13, no. 1
pp. 1 – 11

Abstract

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Abstract Background MYCN amplification is the most important genomic feature in neuroblastoma (NB). However, limited studies have been conducted on the MYCN non-amplified NB including low- and intermediate-risk NB. Here, the genomic characteristics of MYCN non-amplified NB were studied to allow for the identification of biomarkers for molecular stratification. Methods Fifty-eight whole exome sequencing (WES) and forty-eight whole transcriptome sequencing (WTS) samples of MYCN non-amplified NB were analysed. Forty-one patients harboured WES and WTS pairs. Results In the MYCN non-amplified NB WES data, maximum recurrent mutations were found in MUC4 (26%), followed by RBMXL3 (19%), ALB (17%), and MUC16 and SEPD8 (14% each). Two gene fusions, CCDC32-CBX3 (10%) and SAMD5-SASH1 (6%), were recurrent in WTS analysis, and these fusions were detected mostly in non-high-risk patients with ganglioneuroblastoma histology. Analysis of risk-group-specific biomarkers showed that several genes and gene sets were differentially expressed between the risk groups, and some immune-related pathways tended to be activated in the high-risk group. Mutational signatures 6 and 18, which represent DNA mismatch repair associated mutations, were commonly detected in 60% of the patients. In the tumour mutation burden (TMB) analysis, four patients showed high TMB (> 3 mutations/Mb), and had mutations in genes related to either MMR or homologous recombination. Excluding four outlier samples with TMB > 3 Mb, high-risk patients had significantly higher levels of TMB compared with the non-high-risk patients. Conclusions This study provides novel insights into the genomic background of MYCN non-amplified NB. Activation of immune-related pathways in the high-risk group and the results of TMB and mutational signature analyses collectively suggest the need for further investigation to discover potential immunotherapeutic strategies for NB.

Published in BMC Medical Genomics

ISSN: 1755-8794 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine; Science: Biology (General): Genetics
Website: https://bmcmedgenomics.biomedcentral.com

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