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TUMOR-INFILTRATING MACROPHAGE AND MICROVESSEL DENSITY IN ORAL SQUAMOUS CELL CARCINOMA
Bôas, Deise Souza Vilas et al. | Date Issued: 2013
Author
Bôas, Deise Souza Vilas
Takiya, Christina Maeda
Gurgel, Clarissa Araújo Silva
Cabral, Márcia Grillo
Santos, Jean Nunes dos
Affilliation
Federal University of Bahia. Institute of Health Sciences. Department of Biomorphology. Salvador, BA, Brazil / Federal University of Rio de Janeiro. Institute of Biomedical Sciences. Laboratory of Cell Pathology. Rio de Janeiro, RJ, Brazil
Federal University of Rio de Janeiro. Institute of Biomedical Sciences. Laboratory of Cell Pathology. Rio de Janeiro, RJ, Brazil
Fundação Oswaldo Cruz. Centro de Pesquisas Gonçalo Moniz. Programa de Patologia Humana. Salvador, BA, Brasil / Federal University of Bahia. School of Dentistry. Laboratory of Oral Surgical Pathology. Salvador, BA, Brasil
Federal University of Rio de Janeiro. School of Dentistry. Department of Pathology and Oral Diagnosis. Rio de Janeiro, RJ, Brazil
Fundação Oswaldo Cruz. Centro de Pesquisas Gonçalo Moniz. Programa de Patologia Humana. Salvador, BA, Brasil / Federal University of Bahia. School of Dentistry. Laboratory of Oral Surgical Pathology. Salvador, BA, Brasil
Abstract in Portuguese
Macrófagos associados a tumores (MAT) representam o componente principal do estroma de muitos tumores, além de participar da angiogênese tumoral. Este estudo comparou a microdensidade vascular (MDV) e densidade de macrófagos infiltrando o tumor (DMIT) em carcinoma escamocelular da boca (CEC) com diferentes graus histológicos de malignidade. Análise histomorfométrica foi empregada após técnica imuno-histoquímica para os anticorpos fator von-Willebrand e CD68. Uma diferença significante entre MDV e carcinomas bem e moderadamente diferenciados foi observada (p<0,05). MAT estavam fortemente presentes em todos os tumores estudados e a DMIT não foi diferente entre os diferentes graus histológicos de malignidade do CEC (p=0,381). Correlação significante entre MDV e DMIT não foi observada (p=0,870). Em conclusão, os resultados desse estudo sugerem a influência de MAT e angiogênese nos diferentes graus histológicos de malignidade do CEC. Entretanto, a ausência de correlação entre MDV e DMIT sugere que a angiogênese não depende do número de macrófagos presentes neste tipo de câncer, mas do fenótipo predominante. Outros estudos devem ser realizados a fim de contribuir para melhor compreensão da participação de MAT na angiogênese tumoral.
Abstract
Tumor-associated macrophages (TAM) are the main cellular component in stroma of many tumors and participate in tumor angiogenesis. The aim of present study was to compare the microvascular density (MVD) and infiltrating macrophage density (IMD) in oral squamous cell carcinomas (OSCCs) with different histological grades. A histomorphometric analysis was performed after immunohistochemistry using antibodies such as von-Willebrand factor and CD68. A significant difference in MVD was found between well and moderately differentiated OSCCs (p<0.05). TAM were largely present in all studied tumors and the IMD was not different among OSCCs with different histological grades (p=0.381). Significant correlation between MVD and IMD was not observed (p=0.870). In conclusion, these results suggest that TAM and angiogenesis have an influence at different histological grades of OSCC. However, the lack of correlation between MVD and IMD could suggest that angiogenesis does not depend on the number of macrophages present in OSCC, but their predominant phenotype. Further studies involving distinct phenotypes of macrophages should be done to better understand the influence of TAM on the tumor angiogenesis.
Keywords in Portuguese
Angiogênese
Macrófagos
Carcinoma de células escamosas orais
Imuno-histoquímica
 
Keywords
Angiogenesis
Macrophages
Oral squamous cell carcinoma
Immunohistochemistry
 
Publisher
Fundação Odontológica de Ribeirão Preto
Citation
BOAS, D. S. V. et al. Tumor-infiltrating macrophage and microvessel density in oral squamous cell carcinoma. Brazilian Dental Journal, v. 24, n. 3, p. 194-199, 2013.
DOI
10.1590/0103-6440201302049
ISSN
0103-6440