CORRELATION OF IMMUNOHISTOCHEMICAL EXPRESSION OF BETA-CATENIN AND C-MYC WITH AGGRESSIVITY IN GASTRIC TUMORS

Detalhes bibliográficos
Autor(a) principal: Naufel-Junior, Carlos Roberto
Data de Publicação: 2022
Outros Autores: Czeczko, Nicolau Gregori, Malafaia, Osvaldo, Collaço, Luiz, Gasser, Martin, Waaga-Gasser, Ana
Tipo de documento: preprint
Idioma: por
Título da fonte: SciELO Preprints
Texto Completo: https://preprints.scielo.org/index.php/scielo/preprint/view/4139
Resumo: – Background: Biomarkers are macromolecules present in the body that may be related to neoplastic cells. None of them for diagnosis for secondary prevention were defined for gastric cancer. Objective: To investigate the immunohistochemical expression of beta-catenin and c-MYC proteins in gastric cancer and to correlate them with the aggressiveness of gastric tumors. Method: The sample consisted of histopathological slides, stained by H&E and paraffin blocks, and immunostained. Retrospective clinical data were collected. Clinical and epidemiological information was cross-referenced with the result obtained by immunostaining and its statistical analysis. Results: There was a predominance of men (69.1%), with a mean age of 63.8 years, with a predominance of lesions located in the antrum (54.5%), poorly differentiated (49.1%) with signet ring cells in 30 % of cases. On average, 18 lymph nodes were resected and in 30% no affected lymph nodes were detected. In 42.7% there was already distant metastasis, predominantly liver (61.7%). Stage IV was the classification of 43.6%, not being detected angiolymphatic invasion in 77.3% and perineural in 65.5%. Treatment was surgical and chemotherapy in 87.3%, with R0 resection in 79.1%. c-MYC was negative in 99.1% and beta-catenin was not expressed in 90.9%, being inconclusive in 6 cases. Conclusion: The immunohistochemical expression of these proteins in tissues with gastric cancer was not observed. The analyzed biomarkers, c-MYC and beta-catenin, showed no association with tumor aggressiveness in this cancer
id SCI-1_619f770accbd6090cd84acb2dfc4bac8
oai_identifier_str oai:ops.preprints.scielo.org:preprint/4139
network_acronym_str SCI-1
network_name_str SciELO Preprints
repository_id_str
spelling CORRELATION OF IMMUNOHISTOCHEMICAL EXPRESSION OF BETA-CATENIN AND C-MYC WITH AGGRESSIVITY IN GASTRIC TUMORSCORRELAÇÃO DA EXPRESSÃO IMUNOISTOQUíMICA DE BETA-CATENINA E C-MYC COM A AGRESSIVIDADE EM TUMORES DO ESTÔMAGOc-MYCBeta-cateninaCâncer gástrico.Biomarcadores tumoraisc-MYCBeta-cateninGastric cancerTumor biomarkers– Background: Biomarkers are macromolecules present in the body that may be related to neoplastic cells. None of them for diagnosis for secondary prevention were defined for gastric cancer. Objective: To investigate the immunohistochemical expression of beta-catenin and c-MYC proteins in gastric cancer and to correlate them with the aggressiveness of gastric tumors. Method: The sample consisted of histopathological slides, stained by H&E and paraffin blocks, and immunostained. Retrospective clinical data were collected. Clinical and epidemiological information was cross-referenced with the result obtained by immunostaining and its statistical analysis. Results: There was a predominance of men (69.1%), with a mean age of 63.8 years, with a predominance of lesions located in the antrum (54.5%), poorly differentiated (49.1%) with signet ring cells in 30 % of cases. On average, 18 lymph nodes were resected and in 30% no affected lymph nodes were detected. In 42.7% there was already distant metastasis, predominantly liver (61.7%). Stage IV was the classification of 43.6%, not being detected angiolymphatic invasion in 77.3% and perineural in 65.5%. Treatment was surgical and chemotherapy in 87.3%, with R0 resection in 79.1%. c-MYC was negative in 99.1% and beta-catenin was not expressed in 90.9%, being inconclusive in 6 cases. Conclusion: The immunohistochemical expression of these proteins in tissues with gastric cancer was not observed. The analyzed biomarkers, c-MYC and beta-catenin, showed no association with tumor aggressiveness in this cancerRacional: Biomarcadores são macromoléculas presentes no organismo que podem estar relacionadas com células neoplásicas. Nenhum deles para diagnóstico para prevenção secundária foi definido para o câncer gástrico. Objetivo: Investigar a expressão imunoistoquímica das proteínas beta-catenina e c-MYC no câncer gástrico e correlacioná-las com a agressividade dos tumores do estômago. Método: A amostra consistiu em lâminas histopatológicas, coradas por H&E e blocos de parafina, e realizada imunomarcação. Dados clínicos retrospectivos foram coletados. As informações clinicoepidemiológicas foram cruzadas com o resultado obtido pela imunomarcação e sua análise estatística. Resultado: Houve predomínio de homens (69,1%), com idade média de 63,8 anos, predominando lesão localizadaSciELO PreprintsSciELO PreprintsSciELO Preprints2022-05-17info:eu-repo/semantics/preprintinfo:eu-repo/semantics/publishedVersionapplication/pdfhttps://preprints.scielo.org/index.php/scielo/preprint/view/413910.1590/SciELOPreprints.4139porhttps://preprints.scielo.org/index.php/scielo/article/view/4139/7826Copyright (c) 2022 Carlos Roberto Naufel-Junior, Nicolau, Osvaldo Malafaia, Luiz Collaço, Martin Gasser, Ana Waaga-Gasserhttps://creativecommons.org/licenses/by/4.0info:eu-repo/semantics/openAccessNaufel-Junior, Carlos RobertoCzeczko, Nicolau GregoriMalafaia, OsvaldoCollaço, LuizGasser, Martin Waaga-Gasser, Anareponame:SciELO Preprintsinstname:SciELOinstacron:SCI2022-05-16T20:44:41Zoai:ops.preprints.scielo.org:preprint/4139Servidor de preprintshttps://preprints.scielo.org/index.php/scieloONGhttps://preprints.scielo.org/index.php/scielo/oaiscielo.submission@scielo.orgopendoar:2022-05-16T20:44:41SciELO Preprints - SciELOfalse
dc.title.none.fl_str_mv CORRELATION OF IMMUNOHISTOCHEMICAL EXPRESSION OF BETA-CATENIN AND C-MYC WITH AGGRESSIVITY IN GASTRIC TUMORS
CORRELAÇÃO DA EXPRESSÃO IMUNOISTOQUíMICA DE BETA-CATENINA E C-MYC COM A AGRESSIVIDADE EM TUMORES DO ESTÔMAGO
title CORRELATION OF IMMUNOHISTOCHEMICAL EXPRESSION OF BETA-CATENIN AND C-MYC WITH AGGRESSIVITY IN GASTRIC TUMORS
spellingShingle CORRELATION OF IMMUNOHISTOCHEMICAL EXPRESSION OF BETA-CATENIN AND C-MYC WITH AGGRESSIVITY IN GASTRIC TUMORS
Naufel-Junior, Carlos Roberto
c-MYC
Beta-catenina
Câncer gástrico.
Biomarcadores tumorais
c-MYC
Beta-catenin
Gastric cancer
Tumor biomarkers
title_short CORRELATION OF IMMUNOHISTOCHEMICAL EXPRESSION OF BETA-CATENIN AND C-MYC WITH AGGRESSIVITY IN GASTRIC TUMORS
title_full CORRELATION OF IMMUNOHISTOCHEMICAL EXPRESSION OF BETA-CATENIN AND C-MYC WITH AGGRESSIVITY IN GASTRIC TUMORS
title_fullStr CORRELATION OF IMMUNOHISTOCHEMICAL EXPRESSION OF BETA-CATENIN AND C-MYC WITH AGGRESSIVITY IN GASTRIC TUMORS
title_full_unstemmed CORRELATION OF IMMUNOHISTOCHEMICAL EXPRESSION OF BETA-CATENIN AND C-MYC WITH AGGRESSIVITY IN GASTRIC TUMORS
title_sort CORRELATION OF IMMUNOHISTOCHEMICAL EXPRESSION OF BETA-CATENIN AND C-MYC WITH AGGRESSIVITY IN GASTRIC TUMORS
author Naufel-Junior, Carlos Roberto
author_facet Naufel-Junior, Carlos Roberto
Czeczko, Nicolau Gregori
Malafaia, Osvaldo
Collaço, Luiz
Gasser, Martin
Waaga-Gasser, Ana
author_role author
author2 Czeczko, Nicolau Gregori
Malafaia, Osvaldo
Collaço, Luiz
Gasser, Martin
Waaga-Gasser, Ana
author2_role author
author
author
author
author
dc.contributor.author.fl_str_mv Naufel-Junior, Carlos Roberto
Czeczko, Nicolau Gregori
Malafaia, Osvaldo
Collaço, Luiz
Gasser, Martin
Waaga-Gasser, Ana
dc.subject.por.fl_str_mv c-MYC
Beta-catenina
Câncer gástrico.
Biomarcadores tumorais
c-MYC
Beta-catenin
Gastric cancer
Tumor biomarkers
topic c-MYC
Beta-catenina
Câncer gástrico.
Biomarcadores tumorais
c-MYC
Beta-catenin
Gastric cancer
Tumor biomarkers
description – Background: Biomarkers are macromolecules present in the body that may be related to neoplastic cells. None of them for diagnosis for secondary prevention were defined for gastric cancer. Objective: To investigate the immunohistochemical expression of beta-catenin and c-MYC proteins in gastric cancer and to correlate them with the aggressiveness of gastric tumors. Method: The sample consisted of histopathological slides, stained by H&E and paraffin blocks, and immunostained. Retrospective clinical data were collected. Clinical and epidemiological information was cross-referenced with the result obtained by immunostaining and its statistical analysis. Results: There was a predominance of men (69.1%), with a mean age of 63.8 years, with a predominance of lesions located in the antrum (54.5%), poorly differentiated (49.1%) with signet ring cells in 30 % of cases. On average, 18 lymph nodes were resected and in 30% no affected lymph nodes were detected. In 42.7% there was already distant metastasis, predominantly liver (61.7%). Stage IV was the classification of 43.6%, not being detected angiolymphatic invasion in 77.3% and perineural in 65.5%. Treatment was surgical and chemotherapy in 87.3%, with R0 resection in 79.1%. c-MYC was negative in 99.1% and beta-catenin was not expressed in 90.9%, being inconclusive in 6 cases. Conclusion: The immunohistochemical expression of these proteins in tissues with gastric cancer was not observed. The analyzed biomarkers, c-MYC and beta-catenin, showed no association with tumor aggressiveness in this cancer
publishDate 2022
dc.date.none.fl_str_mv 2022-05-17
dc.type.driver.fl_str_mv info:eu-repo/semantics/preprint
info:eu-repo/semantics/publishedVersion
format preprint
status_str publishedVersion
dc.identifier.uri.fl_str_mv https://preprints.scielo.org/index.php/scielo/preprint/view/4139
10.1590/SciELOPreprints.4139
url https://preprints.scielo.org/index.php/scielo/preprint/view/4139
identifier_str_mv 10.1590/SciELOPreprints.4139
dc.language.iso.fl_str_mv por
language por
dc.relation.none.fl_str_mv https://preprints.scielo.org/index.php/scielo/article/view/4139/7826
dc.rights.driver.fl_str_mv https://creativecommons.org/licenses/by/4.0
info:eu-repo/semantics/openAccess
rights_invalid_str_mv https://creativecommons.org/licenses/by/4.0
eu_rights_str_mv openAccess
dc.format.none.fl_str_mv application/pdf
dc.publisher.none.fl_str_mv SciELO Preprints
SciELO Preprints
SciELO Preprints
publisher.none.fl_str_mv SciELO Preprints
SciELO Preprints
SciELO Preprints
dc.source.none.fl_str_mv reponame:SciELO Preprints
instname:SciELO
instacron:SCI
instname_str SciELO
instacron_str SCI
institution SCI
reponame_str SciELO Preprints
collection SciELO Preprints
repository.name.fl_str_mv SciELO Preprints - SciELO
repository.mail.fl_str_mv scielo.submission@scielo.org
_version_ 1797047828522991616