Identification of the Genetic and Clinical Characteristics of Neuroblastomas Using Genome-wide Analysis

Overview

Journal Oncotarget

Specialty Oncology

Date 2018 Jan 4

PMID 29296183

Citations 16

Authors

Kumiko Uryu

Riki Nishimura

Keisuke Kataoka

Yusuke Sato

Atsuko Nakazawa

Hiromichi Suzuki

Kenichi Yoshida

Masafumi Seki

Mitsuteru Hiwatari

Tomoya Isobe

Yuichi Shiraishi

Kenichi Chiba

Hiroko Tanaka

Satoru Miyano

Katsuyoshi Koh

Ryoji Hanada

Akira Oka

Yasuhide Hayashi

Miki Ohira

Takehiko Kamijo

Hiroki Nagase

Tetsuya Takimoto

Tatsuro Tajiri

Akira Nakagawara

Seishi Ogawa

Junko Takita

Affiliations

Soon will be listed here.

Abstract

To provide better insight into the genetic signatures of neuroblastomas, we analyzed 500 neuroblastomas (included specimens from JNBSG) using targeted-deep sequencing for 10 neuroblastoma-related genes and SNP arrays analysis. ALK expression was evaluated using immunohistochemical analysis in 259 samples. Based on genetic alterations, the following 6 subgroups were identified: groups A ( abnormalities), B (other gene mutations), C ( amplification), D (11q loss of heterozygosity [LOH]), E (at least 1 copy number variants), and F (no genetic changes). Groups A to D showed advanced disease and poor prognosis, whereas groups E and F showed excellent prognosis. Intriguingly, in group A, amplification was not a significant prognostic marker, while high ALK expression was a relevant indicator for prognosis ( = 0.033). Notably, the co-existence of amplification and 1p LOH, and the co-deletion of 3p and 11q were significant predictors of relapse ( = 0.043 and = 0.040). Additionally, 6q/8p LOH and 17q gain were promising indicators of survival in patients older than 5 years, and 1p, 4p, and 11q LOH potentially contributed to outcome prediction in the intermediate-risk group. Our genetic overview clarifies the clinical impact of genetic signatures and aids in the better understanding of genetic basis of neuroblastoma.

Citing Articles

Prognostic Value of Molecular Aberrations in Low- or Intermediate-Risk Neuroblastomas: A Systematic Review.

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DNA copy number profiles and systems biology connect chromatin remodeling and DNA repair in high-risk neuroblastoma.

Nascimento T, Poloni J, Thomazini M, Cavalli L, Elifio-Esposito S, Feltes B Genet Mol Biol. 2024; 47(3):e20240007.

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17q Gain in Neuroblastoma: A Review of Clinical and Biological Implications.

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PMID: 38254827 PMC: 10814316. DOI: 10.3390/cancers16020338.

Immunohistochemical expression of anaplastic lymphoma kinase in neuroblastoma and its relations with some clinical and histopathological features.

Phan T, Nguyen T, To N, Thanh T, Ngo D J Pathol Transl Med. 2024; 58(1):29-34.

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Quantitative Diffusion-Weighted MRI of Neuroblastoma.

Abele N, Langner S, Felbor U, Lode H, Hosten N Cancers (Basel). 2023; 15(7).

PMID: 37046600 PMC: 10092990. DOI: 10.3390/cancers15071940.

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