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Suprabasal p53 immunoexpression is strongly associated with high grade dysplasia and risk for malignant transformation in potentially malignant oral lesions from Northern Ireland

机译:基底膜上p53免疫表达与高度发育异常和北爱尔兰潜在恶性口腔病变中发生恶性转化的风险密切相关

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摘要

Aims: No good predictive marker for the malignant transformation of potentially malignant oral lesions (PMOLs) is currently available. This study re-evaluated the value of p53 immunoexpression to predict malignant transformation of PMOLs after discounting possible confounding factors.Methods: PMOLs from 18 patients who showed progression to carcinoma, 16 of the respective carcinomas, and PMOLs from 18 matched controls were evaluated by immunohistochemistry (IHC) for p53 expression. A mouse monoclonal antibody that detects wild-type and mutant forms of human p53 was used. The p53 immunostaining pattern was also correlated with the degree of dysplasia.Results: Suprabasal p53 staining was significantly associated with high grades of dysplasia (p < 0.01). The specificity and positive predictive value (PPV) for malignant transformation of suprabasal p53 staining were superior to the assessment of dysplasia, but sensitivity was inferior. All carcinomas derived from PMOLs with suprabasal p53 showed strong p53 immunostaining. However, the absence of suprabasal p53 staining and/or dysplastic changes did not preclude malignant transformation in a considerable proportion of PMOLs.Conclusions: This study confirms and extends previous findings that suprabasal p53 immunoexpression has a high PPV for malignant transformation of PMOLs and can be used as a specific marker for lesions that are at high risk for malignant transformation. The absence of suprabasal p53 staining (that is, absence of, or basal, p53 staining) is non-informative for prognostic purposes. Because of its limited sensitivity, p53 IHC is not a substitute for the assessment of dysplasia in the evaluation of PMOLs. Instead, p53 IHC emerges as a clinically useful supplement of histopathological assessment in the prognosis of PMOLs.
机译:目的:目前尚无潜在的恶性口腔病变(PMOL)恶变的良好预测指标。这项研究重新评估了p53免疫表达在预测可能的混杂因素后预测PMOLs恶性转化的价值。方法:采用免疫组织化学方法评估了18例进展为癌的患者的PMOLs,16例各自的癌症以及18例匹配对照的PMOLs。 (IHC)用于p53表达。使用小鼠单克隆抗体,其检测人p53的野​​生型和突变形式。 p53免疫染色的模式也与不典型增生的程度有关。结果:基底上p53染色与高度不典型增生显着相关(p <0.01)。基底膜上p53染色恶变的特异性和阳性预测值(PPV)优于发育异常的评估,但敏感性较差。所有源自基底上p53的PMOL的癌均表现出强烈的p53免疫染色。然而,缺乏上基底p53染色和/或增生异常改变并不排除相当一部分PMOLs发生恶性转化。用作恶性转化高风险病变的特异性标志物。基底膜上p53染色的缺乏(即p53染色的缺乏或基础)对于预后目的是无意义的。由于其敏感性有限,因此p53 IHC不能替代PMOLs评估中的发育异常评估。取而代之的是,p53 IHC成为组织病理学评估对PMOLs预后的临床有用补充。

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