Mutations, Differential Gene Expression, and Chimeric Transcripts in Esophageal Squamous Cell Carcinoma Show High Heterogeneity

Paulo Thiago de Souza-Santos; Sheila Coelho Soares Lima; Pedro Nicolau-Neto; Mariana Boroni; Nathalia Meireles Da Costa; Lilian Brewer; Albert Nobre Menezes; Carolina Furtado; Miguel Angelo Martins Moreira; Hector N. Seuanez; Tatiana de Almeida Simão; Luis Felipe Ribeiro Pinto

Translational Oncology (Dec 2018)

Mutations, Differential Gene Expression, and Chimeric Transcripts in Esophageal Squamous Cell Carcinoma Show High Heterogeneity

Paulo Thiago de Souza-Santos,
Sheila Coelho Soares Lima,
Pedro Nicolau-Neto,
Mariana Boroni,
Nathalia Meireles Da Costa,
Lilian Brewer,
Albert Nobre Menezes,
Carolina Furtado,
Miguel Angelo Martins Moreira,
Hector N. Seuanez,
Tatiana de Almeida Simão,
Luis Felipe Ribeiro Pinto

Affiliations

Paulo Thiago de Souza-Santos: Molecular Carcinogenesis Program, Instituto Nacional de Câncer–INCA, Rua Andre Cavalcanti, 37–6° andar, Centro, Rio de Janeiro, RJ, Brasil, 20231-050
Sheila Coelho Soares Lima: Molecular Carcinogenesis Program, Instituto Nacional de Câncer–INCA, Rua Andre Cavalcanti, 37–6° andar, Centro, Rio de Janeiro, RJ, Brasil, 20231-050
Pedro Nicolau-Neto: Molecular Carcinogenesis Program, Instituto Nacional de Câncer–INCA, Rua Andre Cavalcanti, 37–6° andar, Centro, Rio de Janeiro, RJ, Brasil, 20231-050
Mariana Boroni: Bioinformatics and Computational Biology Laboratory, Instituto Nacional de Câncer–INCA, Rua Andre Cavalcanti, 37–1° andar, Centro, Rio de Janeiro, RJ, Brasil, 20231-050
Nathalia Meireles Da Costa: Molecular Carcinogenesis Program, Instituto Nacional de Câncer–INCA, Rua Andre Cavalcanti, 37–6° andar, Centro, Rio de Janeiro, RJ, Brasil, 20231-050
Lilian Brewer: Biochemistry Department, Instituto de Biologia Roberto Alcântara Gomes, Universidade do Estado do Rio de Janeiro, Boulevard 28 de Setembro, 77-Maracanã, Rio de Janeiro, RJ, Brasil, 20551-030
Albert Nobre Menezes: College of Medical and Dental Sciences, University of Birmingham, Vicent Drive, Edgbaston, Birmingham, B15 2TT, UK
Carolina Furtado: Genetics Program, Instituto Nacional de Câncer–INCA, Rua Andre Cavalcanti, 37–4° andar, Centro, Rio de Janeiro, RJ, Brasil, 20231-050
Miguel Angelo Martins Moreira: Genetics Program, Instituto Nacional de Câncer–INCA, Rua Andre Cavalcanti, 37–4° andar, Centro, Rio de Janeiro, RJ, Brasil, 20231-050
Hector N. Seuanez: Genetics Program, Instituto Nacional de Câncer–INCA, Rua Andre Cavalcanti, 37–4° andar, Centro, Rio de Janeiro, RJ, Brasil, 20231-050
Tatiana de Almeida Simão: Biochemistry Department, Instituto de Biologia Roberto Alcântara Gomes, Universidade do Estado do Rio de Janeiro, Boulevard 28 de Setembro, 77-Maracanã, Rio de Janeiro, RJ, Brasil, 20551-030
Luis Felipe Ribeiro Pinto: Molecular Carcinogenesis Program, Instituto Nacional de Câncer–INCA, Rua Andre Cavalcanti, 37–6° andar, Centro, Rio de Janeiro, RJ, Brasil, 20231-050; Biochemistry Department, Instituto de Biologia Roberto Alcântara Gomes, Universidade do Estado do Rio de Janeiro, Boulevard 28 de Setembro, 77-Maracanã, Rio de Janeiro, RJ, Brasil, 20551-030; Address all correspondence to: Luis Felipe Ribeiro Pinto, Rua Andre Cavalcanti, 37–6° andar, Centro, Rio de Janeiro, RJ, Brasil, 20231-050.

Journal volume & issue: Vol. 11, no. 6
pp. 1283 – 1291

Abstract

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Esophageal squamous cell carcinoma (ESCC) is a frequent and lethal neoplasia. As recent advances in targeted therapy have not improved ESCC prognosis, characterization of molecular alterations associated to this tumor is of foremost relevance. In this study, we analyze, for the first time, the complete genomic profile of ESCC by RNA-seq. TP53 was the most frequently mutated gene in the investigation and validation sets (78.6% and 67.4%, respectively). Differential expression analysis between tumor and nontumor adjacent mucosa showed 6698 differentially expressed genes, most of which were overexpressed (74%). Enrichment analysis identified overrepresentation of Wnt pathway, with overexpressed activators and underexpressed inactivators, suggesting activation of canonical and noncanonical Wnt signaling pathways. Higher WNT7B expression was associated with poor prognosis. Twenty-one gene fusions were identified in 50% of tumors, none of which involving the same genes in different patients; 71% of fusions involved syntenic genes. Comparisons with TCGA data showed co-amplification of seven gene pairs involved in fusions in the present study (~33%), suggesting that these rearrangements might have been driven by chromoanagenesis. In conclusion, genomic alterations in ESCC are highly heterogeneous, impacting negatively in target therapy development.

Published in Translational Oncology

ISSN: 1944-7124 (Print); 1936-5233 (Online)
Publisher: Elsevier
Country of publisher: Netherlands
LCC subjects: Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens
Website: https://www.journals.elsevier.com/translational-oncology/

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