头颈部鳞状细胞癌中p53过表达:文献综述

H. Raybaud-Diogène , B. Tétu , R. Morency , A. Fortin , R.A. Monteil
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引用次数: 143

摘要

作为一种肿瘤抑制基因,p53的失活诱导了许多人类癌症的发展。p53突变与头颈部鳞状细胞癌(HN-SCC)的发病机制有关,且发病率高。在癌前病变和原位癌中,p53过表达不仅局限于肿瘤细胞,而且经常影响p53阳性肿瘤附近正常的角质形成细胞或存在于发育不良区域。这些结果表明,作为HN-SCC发展早期阶段的参与者,p53改变可能是指示特定口腔癌前病变倾向于恶性肿瘤的优秀生物标志物。在大多数情况下,肿瘤转移的p53过表达状态与原发肿瘤的p53过表达状态相同,表明p53突变先于转移扩散。在多发性原发肿瘤患者中,在远离肿瘤的上皮细胞中观察到多个p53过表达灶。因此,p53在正常上皮中的表达表明转化为第二或第三原发癌症的风险增加。在同一患者的不同原发肿瘤中,不同的p53突变表明这些癌症是作为独立事件发生的;这些结果支持多焦点多克隆过程的存在。尽管上述结果支持p53作为有效的肿瘤生物标志物,但大多数研究表明p53的表达与临床和组织病理学参数之间没有关系。p53突变在HN-SCC的进展和重要预后中的作用尚未得到证实。
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p53 overexpression in head and neck squamous cell carcinoma: Review of the literature

As a tumour suppressor gene, the inactivation of p53 induces the development of numerous human cancers. Mutations of p53 have been implicated in the pathogenesis of head and neck squamous cell carcinoma (HN-SCC) at a high incidence. In premalignant lesions and in situ carcinomas, p53 overexpression is not exclusively restricted to neoplastic cells, but frequently affects the normal appearing keratinocytes adjacent to p53 positive neoplasms or present in dysplastic areas. These results suggest that as contributors to the early phases of HN-SCC development, p53 alterations may be excellent biomarkers that indicate the predisposition of a particular oral cavity premalignant lesion toward malignancy. In most cases, the p53 overexpression status of a tumour metastasis is identical to that of a primary tumour, indicating that a p53 mutation precedes metastatic spread. In patients with multiple primary tumours, multiple foci of p53 overexpression are observed in epithelia distant from the tumour. So the expression of p53 in normal epithelium would indicate an increased risk for transformation to second or third primary cancers. Distinct p53 mutations in different primary tumours of the same patient indicate that these cancers arise as independent events; these results support the existence of multifocal polyclonal processes. Regardless of the aforementioned results that support p53 as a valid tumour biomarker, most studies have shown no relationship between the expression of p53 and clinical and histopathological parameters. The role played by p53 mutations in the progression and vital prognosis of HN-SCC has not yet been demonstrated.

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