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p53过表达的免疫组织化学测定。一种识别浅表性膀胱癌进展的简便易行的方法?

Immunohistochemical determination of p53 overexpression. An easy and readily available method to identify progression in superficial bladder cancer?

作者信息

Burkhard F C, Markwalder R, Thalmann G N, Studer U E

机构信息

Department of Urology, University of Berne, Inselspital, Switzerland.

出版信息

Urol Res. 1997;25 Suppl 1:S31-5. doi: 10.1007/BF00942045.

Abstract

Overexpression of p53, as determined by immunohistochemical staining with the murine monoclonal antibody DO7, was determined in specimens of 46 primary superficial transitional cell bladder tumours (14 TaG2, 10 T1G2, 22 T1G3). A colon cancer specimen served as a positive control and normal mesenchymal cells in the specimens served as an internal negative control. An exceptionally high proportion 36/46 (78%) of the specimens were found to stain positively for p53 in over 20% of the cell nuclei. After a median follow-up of 7 years, ten patients developed progressive disease. Of these ten patients nine demonstrated p53 positivity, resulting in a sensitivity of 90%. However, 27 of the overall 36 patients (75%) with p53-positive tumours did not progress to a higher stage or metastatic disease. These findings suggest that p53 overexpression is not of predictive prognostic value in superficial transitional cell carcinoma. With 7 of 14 specimens (50%) of Ta tumours overexpressing p53, the results were suggestive of p53 mutation being an early event in carcinogenesis. When the threshold was set at 50% of the cell nuclei overexpressing p53, 16/46 (35%) classified as p53 positive. Of the 16 tumours staining positively for p53, 7 (46%) progressed and 9 (56%) did not. None of the Ta and 16 (50%) of the T1 tumours classified as positive. This more stringent definition of positivity still does not identify p53 positivity as a single prognostic factor. With 50% of T1 tumours classifying as positive, we still find that p53 mutation may be an early event in carcinogenesis of bladder cancer.

摘要

采用鼠单克隆抗体DO7进行免疫组织化学染色,检测了46例原发性浅表性移行细胞膀胱癌标本(14例TaG2、10例T1G2、22例T1G3)中p53的过表达情况。取一份结肠癌标本作为阳性对照,标本中的正常间充质细胞作为内源性阴性对照。结果发现,高达36/46(78%)的标本中,超过20%的细胞核p53染色呈阳性。中位随访7年后,10例患者出现疾病进展。在这10例患者中,9例p53呈阳性,敏感性为90%。然而,在36例p53阳性肿瘤患者中,有27例(75%)未进展至更高分期或发生转移。这些结果表明,p53过表达在浅表性移行细胞癌中并无预测预后的价值。14例Ta肿瘤标本中有7例(50%)p53过表达,提示p53突变可能是致癌过程中的早期事件。当将p53过表达细胞核的阈值设定为50%时,46例中有16例(35%)被归类为p53阳性。在16例p53染色阳性的肿瘤中,7例(46%)发生进展,9例(56%)未进展。Ta肿瘤均为阴性,16例(50%)T1肿瘤被归类为阳性。这种对阳性更为严格的定义仍无法将p53阳性确定为单一的预后因素。尽管50%的T1肿瘤被归类为阳性,但我们仍发现p53突变可能是膀胱癌致癌过程中的早期事件。

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