Remvikos Y, Tominaga O, Hammel P, Laurent-Puig P, Salmon R J, Dutrillaux B, Thomas G
Laboratoire de Radiopathologie, URA 620, Institute Curie, Paris, France.
Br J Cancer. 1992 Oct;66(4):758-64. doi: 10.1038/bjc.1992.352.
Allelic losses on the short arm of chromosome 17 occur frequently in colorectal cancers. Despite the existence of other common molecular events such as loss of the long arms of chromosomes 18 and 5, it has been demonstrated that the former has the greatest prognostic significance. Of the various genes mapping to the commonly deleted sequence, the best candidate as a 'target' seems to be the p53 antioncogene. We applied our methods of detection of the p53 protein in a series of 78 colorectal cancers stored in a tumour bank from 1985 to 1989, for which the median follow-up was 42 months. Nuclear-attached p53 was quantified by flow cytometry and soluble p53 was assayed by ELISA. Both assays used a monoclonal antibody considered to be specific for a conformational epitope present only on the mutated protein. Fifty of the 78 tumours (64%) were found to present significant levels of p53 attached to the nucleus. A further two tumours contained high levels of p53 only in their soluble fraction. Thus, 52 out of 78 cancers (67%) were considered to be positive for p53. The p53 content correlated with 17p loss (P < 0.002), hyperdiploid DNA content (P < 0.001) and tumour site (P < 0.03), but not Dukes' stage (P = 0.15). p53 negative cases had a better overall survival than p53 positive ones (P < 0.03). When the 14 stage D tumours were excluded from the analysis, p53 was no longer significantly predictive of survival (P < 0.07), but remained predictive of recurrence (P < 0.02) and metastasis (P < 0.03). Multivariate analysis was not performed because of the small number of cases. Overall, disease-free and metastasis-free survival were compared to the positivity obtained either with pAb 421 and/or 1801 or pAb 240 since all three were used in the flow cytometric analysis, defining subsets of 421-, 1801+ and 421-, 1801-, 240+. The presence of nuclear protein presenting the mutation-specific epitope, recognised by pAb 240, was found to be the most discriminant. It must be noted that univariate survival analysis demonstrated that more than 80% of patients with p53-negative tumours were alive at 3 years vs less than 50% in the p53-positive group. A large prospective study should be conducted to define the exact prognostic significance of the p53 content of colorectal carcinomas.
17号染色体短臂上的等位基因缺失在结直肠癌中频繁发生。尽管存在其他常见的分子事件,如18号和5号染色体长臂缺失,但已证明前者具有最大的预后意义。在定位于常见缺失序列的各种基因中,作为“靶点”的最佳候选基因似乎是p53抑癌基因。我们应用检测p53蛋白的方法,对1985年至1989年储存在肿瘤库中的一系列78例结直肠癌进行检测,这些病例的中位随访时间为42个月。通过流式细胞术对核附着的p53进行定量,通过酶联免疫吸附测定法检测可溶性p53。两种检测方法均使用一种单克隆抗体,该抗体被认为对仅存在于突变蛋白上的构象表位具有特异性。78例肿瘤中有50例(64%)被发现核附着的p53水平显著升高。另外2例肿瘤仅在其可溶部分含有高水平的p53。因此,78例癌症中有52例(67%)被认为p53呈阳性。p53含量与17p缺失(P<0.002)、超二倍体DNA含量(P<0.001)和肿瘤部位(P<0.03)相关,但与Dukes分期无关(P=0.15)。p53阴性病例的总生存期优于p53阳性病例(P<0.03)。当分析中排除14例D期肿瘤时,p53不再是生存的显著预测指标(P<0.07),但仍然是复发(P<0.02)和转移(P<0.03)的预测指标。由于病例数量较少,未进行多变量分析。总体而言,将无病生存期和无转移生存期与使用pAb 421和/或1801或pAb 240获得的阳性结果进行比较,因为在流式细胞术分析中使用了这三种抗体,定义了421+、1801+和421-、1801-、240+亚组。发现被pAb 240识别的呈现突变特异性表位的核蛋白的存在最具鉴别力。必须指出的是,单变量生存分析表明,p53阴性肿瘤患者3年生存率超过80%,而p53阳性组则不到50%。应该进行一项大型前瞻性研究,以确定结直肠癌中p53含量的确切预后意义。
