Please use this identifier to cite or link to this item: https://ninho.inca.gov.br/jspui/handle/123456789/6262
Title: Multi-cancer V-ATPase molecular signatures: A distinctive balance of subunit C isoforms in esophageal carcinoma
Authors: Vieira, Juliana Couto
Nicolau Neto, Pedro
Costa, Evenilton Pessoa
Figueira, Frederico Firme
Simão, Tatiana de Almeida
Façanha, Anna Lvovna Okorokova
Pinto, Luis Felipe Ribeiro
Façanha, Arnoldo Rocha
Keywords: Biomarkers, Tumor
Cancer Biomarker
Esophageal Neoplasms
Esophageal Cancer
Vacuolar Proton
Translocating ATPases
Issue Date: Jan-2020
Publisher: EBioMedicine
Abstract: Background: V-ATPases are hetero-oligomeric enzymes consisting of 13 subunits and playing key roles in ion homeostasis and signaling. Differential expression of these proton pumps has been implicated in carcinogenesis and metastasis. To elucidate putative molecular signatures underlying these phenomena, we evaluated the expression of V-ATPase genes in esophageal squamous cell carcinoma (ESCC) and extended the analysis to other cancers. Methods: Expression of all V-ATPase genes were analyzed in ESCC by a microarray data and in different types of tumors available from public databases. Expression of C isoforms was validated by qRT-PCR in paired ESCC samples. Findings: A differential expression pattern of V-ATPase genes was found in different tumors, with combinations in up- and down-regulation leading to an imbalance in the expression ratios of their isoforms. Particularly, a high C1 and low C2 expression pattern accurately discriminated ESCC from normal tissues. Structural modeling of C2a isoform uncovered motifs for oncogenic kinases in an additional peptide stretch, and an actin-biding domain downstream to this sequence. Interpretation: Altogether these data revealed that the expression ratios of subunits/isoforms could form a conformational code that controls the H+ pump regulation and interactions related to tumorigenesis. This study establishes a paradigm change by uncovering multi-cancer molecular signatures present in the V-ATPase structure, from which future studies must address the complexity of the onco-related V-ATPase assemblies as a whole, rather than targeting changes in specific subunit
URI: http://sr-vmlxaph03:8080/jspui/handle/123456789/6262
ISSN: 2352-3964
Appears in Collections:Artigo de Periódicos da Pesquisa Clínica



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