ETV4 plays a role on the primary events during the adenoma-adenocarcinoma progression in colorectal cancer

Aline Simoneti Fonseca; Anelisa Ramão; Matheus Carvalho Bürger; Jorge Estefano Santana de Souza; Dalila Lucíola Zanette; Greice Andreotti de Molfetta; Luíza Ferreira de Araújo; Rafaela de Barros e Lima Bueno; Graziela Moura Aguiar; Jéssica Rodrigues Plaça; Cleidson de Pádua Alves; Anemari Ramos Dinarte dos Santos; Daniel Onofre Vidal; Gyl Eanes Barros Silva; Rodrigo Alexandre Panepucci; Fernanda Maris Peria; Omar Féres; José Joaquim Ribeiro da Rocha; Marco A. Zago; Wilson A. Silva

doi:10.1186/s12885-021-07857-x

ETV4 plays a role on the primary events during the adenoma-adenocarcinoma progression in colorectal cancer

Aline Simoneti Fonseca(Universidade de São Paulo), Anelisa Ramão(Universidade de São Paulo), Matheus Carvalho Bürger, Jorge Estefano Santana de Souza, Dalila Lucíola Zanette(Universidade de Ribeirão Preto), Greice Andreotti de Molfetta(Universidade de Ribeirão Preto), Luíza Ferreira de Araújo(Universidade de Ribeirão Preto), Rafaela de Barros e Lima Bueno(Universidade de São Paulo), Graziela Moura Aguiar, Jéssica Rodrigues Plaça, Cleidson de Pádua Alves, Anemari Ramos Dinarte dos Santos, Daniel Onofre Vidal, Gyl Eanes Barros Silva(Hospital Universitário da Universidade Federal do Maranhão), Rodrigo Alexandre Panepucci, Fernanda Maris Peria(Universidade de São Paulo), Omar Féres(Universidade de São Paulo), José Joaquim Ribeiro da Rocha(Universidade de São Paulo), Marco A. Zago, Wilson A. Silva(Universidade de Ribeirão Preto)

BMC Cancer

March 1, 2021

10.1186/s12885-021-07857-x

Cited by 23Open Access

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Abstract

BACKGROUND: Colorectal cancer (CRC) is one of the most common cancers worldwide; it is the fourth leading cause of death in the world and the third in Brazil. Mutations in the APC, DCC, KRAS and TP53 genes have been associated with the progression of sporadic CRC, occurring at defined pathological stages of the tumor progression and consequently modulating several genes in the corresponding signaling pathways. Therefore, the identification of gene signatures that occur at each stage during the CRC progression is critical and can present an impact on the diagnosis and prognosis of the patient. In this study, our main goal was to determine these signatures, by evaluating the gene expression of paired colorectal adenoma and adenocarcinoma samples to identify novel genetic markers in association to the adenoma-adenocarcinoma stage transition. METHODS: Ten paired adenoma and adenocarcinoma colorectal samples were subjected to microarray gene expression analysis. In addition, mutations in APC, KRAS and TP53 genes were investigated by DNA sequencing in paired samples of adenoma, adenocarcinoma, normal tissue, and peripheral blood from ten patients. RESULTS: Gene expression analysis revealed a signature of 689 differentially expressed genes (DEG) (fold-change> 2, p< 0.05), between the adenoma and adenocarcinoma paired samples analyzed. Gene pathway analysis using the 689 DEG identified important cancer pathways such as remodeling of the extracellular matrix and epithelial-mesenchymal transition. Among these DEG, the ETV4 stood out as one of the most expressed in the adenocarcinoma samples, further confirmed in the adenocarcinoma set of samples from the TCGA database. Subsequent in vitro siRNA assays against ETV4 resulted in the decrease of cell proliferation, colony formation and cell migration in the HT29 and SW480 colorectal cell lines. DNA sequencing analysis revealed KRAS and TP53 gene pathogenic mutations, exclusively in the adenocarcinomas samples. CONCLUSION: Our study identified a set of genes with high potential to be used as biomarkers in CRC, with a special emphasis on the ETV4 gene, which demonstrated involvement in proliferation and migration.

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