Gene Expression and Molecular Pathway Activation Signatures of -amplified Neuroblastomas

Overview

Journal Oncotarget

Specialty Oncology

Date 2017 Nov 16

PMID 29137381

Citations 14

Authors

Ivan Petrov

Maria Suntsova

Elena Ilnitskaya

Sergey Roumiantsev

Maxim Sorokin

Andrew Garazha

Pavel Spirin

Timofey Lebedev

Nurshat Gaifullin

Sergey Larin

Olga Kovalchuk

Dmitry Konovalov

Vladimir Prassolov

Alexander Roumiantsev

Anton Buzdin

Affiliations

Soon will be listed here.

Abstract

Neuroblastoma is a pediatric cancer arising from sympathetic nervous system. Remarkable heterogeneity in outcomes is one of its widely known features. One of the traits strongly associated with the unfavorable subtype is the amplification of oncogene . Here, we performed cross-platform biomarker detection by comparing gene expression and pathway activation patterns from the two literature reports and from our experimental dataset, combining profiles for the 761 neuroblastoma patients with known amplification status. We identified 109 / 25 gene expression / pathway activation biomarkers strongly linked with the amplification. The marker genes/pathways are involved in the processes of purine nucleotide biosynthesis, ATP-binding, tetrahydrofolate metabolism, building mitochondrial matrix, biosynthesis of amino acids, tRNA aminoacylation and NADP-linked oxidation-reduction processes, as well as in the tyrosine phosphatase activity, p53 signaling, cell cycle progression and the G1/S and G2/M checkpoints. To connect molecular functions of the genes involved in -amplified phenotype, we built a new molecular pathway using known intracellular protein interaction networks. The activation of this pathway was highly selective in discriminating -amplified neuroblastomas in all three datasets. Our data also suggest that the phosphoinositide 3-kinase (PI3K) inhibitors may provide new opportunities for the treatment of the -amplified neuroblastoma subtype.

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