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免疫组化检测p53肿瘤抑制基因蛋白过表达与高增殖性人乳腺腺癌预后的关系

Association of immunohistochemical p53 tumor suppressor gene protein overexpression with prognosis in highly proliferative human mammary adenocarcinomas.

作者信息

Schimmelpenning H, Eriksson E T, Zetterberg A, Auer G U

机构信息

Department of General Surgery, Johann-Wolfgang Goethe University Hospital, Frankfurt, Germany.

出版信息

World J Surg. 1994 Nov-Dec;18(6):827-32; discussion 832-3. doi: 10.1007/BF00299077.

Abstract

An increasing body of evidence suggests that in addition to conventional histopathologic tumor characteristics, DNA content measurements, cell kinetic data, and investigations of tumor suppressor gene expressions might be of valuable information in breast cancer patients. Against this background we investigated immunohistochemically overexpression of the interphase associated protein proliferating cell nuclear antigen (PCNA) and the mutant p53 protein in routinely paraffin-embedded surgical specimens from 180 breast cancer patients with known nuclear DNA profiles. The mean clinical follow-up was 16 years (range 13-20 years). The percentage of PCNA immunoreactive tumor cell nuclei ranged between < 5% and 60% (mean 13.59 +/- 10.85%). There was a direct association between high levels of PCNA expression (> 20%) and p53 protein overexpression (p = 0.001), high histologic tumor grade (p = 0.009), and DNA aneuploidy (p = 0.019). Mutant p53 protein overexpression was found in 44 of 180 (24%) cases and was significantly related to high histologic tumor grade (p = 0.004), DNA aneuploidy (p = 0.001), and high levels of PCNA expression (p = 0.001). Patients with highly proliferative carcinomas (> 20% PCNA expression) had a shortened distant metastases-free survival when their neoplasms overexpressed p53. In contrast, the distant metastases-free survival of patients with highly proliferative, p53-negative tumors was significantly longer (p = 0.03). Immunohistochemical p53 protein overexpression thus appears to be indicative of an increased malignant potential in breast cancer patients. Highly proliferative tumors composed of p53 immunoreactive neoplastic cells clinically seem to behave more aggressively than the highly proliferative p53-negative tumors.

摘要

越来越多的证据表明,除了传统的组织病理学肿瘤特征外,DNA含量测量、细胞动力学数据以及肿瘤抑制基因表达研究可能对乳腺癌患者具有重要信息价值。在此背景下,我们采用免疫组织化学方法研究了180例已知核DNA谱的乳腺癌患者常规石蜡包埋手术标本中与间期相关的增殖细胞核抗原(PCNA)和突变型p53蛋白的过表达情况。平均临床随访时间为16年(范围13 - 20年)。PCNA免疫反应性肿瘤细胞核的百分比在<5%至60%之间(平均13.59±10.85%)。PCNA高表达水平(>20%)与p53蛋白过表达(p = 0.001)、高组织学肿瘤分级(p = 0.009)和DNA非整倍体(p = 0.019)之间存在直接关联。在180例(24%)病例中有44例发现突变型p53蛋白过表达,且与高组织学肿瘤分级(p = 0.004)、DNA非整倍体(p = 0.001)和PCNA高表达水平(p = 0.001)显著相关。当肿瘤过表达p53时,具有高增殖性癌(PCNA表达>20%)的患者无远处转移生存期缩短。相反,具有高增殖性、p53阴性肿瘤的患者无远处转移生存期明显更长(p = 0.03)。因此,免疫组织化学p53蛋白过表达似乎表明乳腺癌患者的恶性潜能增加。由p53免疫反应性肿瘤细胞组成的高增殖性肿瘤在临床上似乎比高增殖性p53阴性肿瘤表现得更具侵袭性。

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