Microvascular density and tumor budding in oral squamous cell carcinoma.

E-M Assis, M Rodrigues, J-C Vieira, M-I Pascoaloti, H-M Júnior, G-R Souto, P-E Souza, M-C Horta
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引用次数: 3

Abstract

Background: 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.

Material and methods: 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.

Results: 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). This difference was not observed when MVD was assessed by immunostaining for CD105 (p > 0.05).

Conclusions: 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.

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口腔鳞状细胞癌微血管密度与肿瘤出芽。
背景:口腔鳞状细胞癌(Oral squamous cell carcinoma, OSCC)是除非黑色素瘤皮肤癌外最常见的头颈部恶性肿瘤。尽管最近在诊断和治疗方面取得了进展,但这种疾病的死亡率仍然很高。孤立的肿瘤细胞或在肿瘤侵袭前部出现多达4个细胞的小簇,称为肿瘤出芽,与OSCC较差的预后相关。血管生成也被认为是恶性肿瘤进展和转移发展的决定性因素。几项研究调查了微血管密度(MVD)作为OSCC潜在预后因素的评估。本研究旨在评估在OSCC中,高强度肿瘤出芽与低强度或无肿瘤出芽的肿瘤之间MVD的差异。在高强度肿瘤出芽的样品中,还评估了出芽区域和出芽外区域之间MVD的差异。此外,该研究还评估了MVD在性别、年龄、吸烟、肿瘤位置和肿瘤大小等临床病理特征方面的差异。材料和方法:150[150]份OSCC样本进行免疫组化,评估肿瘤出芽强度(通过多细胞角蛋白免疫染色)和MVD(通过CD34和CD105免疫染色,独立)。使用描述性和分析性统计对数据进行处理。结果:免疫染色CD34、CD105评价MVD在性别、年龄、吸烟情况、肿瘤部位、肿瘤大小等临床病理特征上无显著差异(p > 0.05)。通过免疫染色CD34或CD105评估,高强度肿瘤出芽的肿瘤与低强度或无肿瘤出芽的肿瘤相比,MVD无差异(p > 0.05)。然而,在高强度肿瘤出芽的样本中,CD34免疫染色评估的MVD在出芽区域高于出芽区域外的区域(p < 0.05)。用CD105免疫染色法检测MVD时,没有观察到这种差异(p > 0.05)。结论:出芽区较高的MVD可能是一个额外的迹象,表明这是肿瘤的一个特殊区域,与肿瘤进展相关的生物学现象有关。
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来源期刊
CiteScore
4.50
自引率
0.00%
发文量
52
期刊介绍: 1. Oral Medicine and Pathology: Clinicopathological as well as medical or surgical management aspects of diseases affecting oral mucosa, salivary glands, maxillary bones, as well as orofacial neurological disorders, and systemic conditions with an impact on the oral cavity. 2. Oral Surgery: Surgical management aspects of diseases affecting oral mucosa, salivary glands, maxillary bones, teeth, implants, oral surgical procedures. Surgical management of diseases affecting head and neck areas. 3. Medically compromised patients in Dentistry: Articles discussing medical problems in Odontology will also be included, with a special focus on the clinico-odontological management of medically compromised patients, and considerations regarding high-risk or disabled patients. 4. Implantology 5. Periodontology
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