Microvascular density and tumor budding in oral squamous cell carcinoma

6533b86dfe1ef96bd12c97c0

RESEARCH PRODUCT

Microvascular density and tumor budding in oral squamous cell carcinoma

Eliene Magda De Assis Mayara Rodrigues Jéssica Campos Vieira Maria Inês Mantuani Pascoaloti Helvécio Marangon Júnior Giovanna Ribeiro Souto Paulo Eduardo Alencar Souza Martinho Campolina Rebello Horta

subject

allograft Otorhinolaryngology injury alveolar inferior nerve Surgery General Dentistry UNESCO:CIENCIAS MÉDICAS decellularized allograft

description

Oral squamous cell carcinoma (OSCC) is the most prevalent malignant head and neck tumor, excluding the nonmelanoma skin cancer. Despite recent advances in the diagnosis and treatment, the disease's mortality rate is nonetheless high. The presence of isolated neoplastic cells or small clusters of up to four cells at the tumor?s invasive front, named tumor budding, is associated with a worse prognosis in OSCC. Angiogenesis has also been recognized as a determining factor in the progression of malignancies and in the development of metastases. Several studies have investigated the assessment of microvascular density (MVD) as a potential prognostic factor in OSCC. This study aimed to evaluate, in OSCC, differences in MVD between tumors with high-intensity tumor budding and tumors with low-intensity or no tumor budding. In samples with high-intensity tumor budding, differences in MVD between the budding area and the area outside the budding were also evaluated. Moreover, the study assessed differences in MVD concerning clinicopathological characteristics such as sex, age, tobacco smoking, tumor location and tumor size. One hundred and fifty [150] samples of OSCC were subjected to immunohistochemistry to assess the intensity of tumor budding (by immunostaining for multi-cytokeratin) and MVD (by immunostaining for CD34 and CD105, independently). The data were treated using descriptive and analytical statistics. There were no differences in MVD, assessed by immunostaining for CD34 or CD105, concerning clinicopathological characteristics such as sex, age, tobacco smoking, tumor location and tumor size (p > 0.05). Tumors with high-intensity tumor budding did not show differences in MVD, assessed by immunostaining for CD34 or CD105, when compared to tumors with low-intensity or no tumor budding (p > 0.05). However, in samples with high-intensity tumor budding, the MVD assessed by immunostaining for CD34 was higher in the budding area than in the area outside the budding (p 0.05). The higher MVD in the budding area may be an additional indication that this is a peculiar region of the tumor, associated with biological phenomena related to tumor progression.

year	journal	country	edition	language
2022-08-14	Medicina Oral Patología Oral y Cirugia Bucal

https://doi.org/10.4317/medoral.25640