Micelli G, Donadeo A, Quaranta M
Clinical-Chemistry Laboratory, Oncology Institute, Bari, Italy.
Cell Biophys. 1992 Aug-Dec;21(1-3):25-31. doi: 10.1007/BF02789475.
p53 was originally considered to be a nuclear oncogene, but several convergent lines of research have indicated that the wild-type gene functions as a tumor suppressor gene negatively regulating the cell cycle. Mutations in the p53 gene have been detected in many tumor types and seem to be the most common genetic alterations in human cancer. In this preliminary study, sera of 92 patients (pts) with breast disease were analyzed for the presence of the mutant p53 protein (mp53) with a selective immunoenzyme assay employing a monoclonal antibody (PAb 240) specific for the majority of mammalian m p53 but not for the wild-type protein. Of the 10 patients with benign breast disease, only two (20%) showed detectable m p53 levels in the serum. In the breast cancer group, sera from 7 of the 30 pts (23%) without lymph node involvement were positive for m p53, as were 7 out of the 45 pts (15%) with metastatic lymph nodes and 1 out of the 7 pts (14%) with disseminated disease. The specificity of m p53 assay evaluated in 20 healthy controls was 100%. These preliminary results showed that serum positivity for m p53 is not related to breast disease extension. Further studies to assess the utility of m p53 as a possible prognosis factor in breast cancer are currently in progress.
p53最初被认为是一种核癌基因,但多项研究结果表明,野生型基因作为肿瘤抑制基因,对细胞周期起负调控作用。在许多肿瘤类型中都检测到了p53基因的突变,这些突变似乎是人类癌症中最常见的基因改变。在这项初步研究中,采用一种单克隆抗体(PAb 240)的选择性免疫酶测定法,分析了92例乳腺疾病患者血清中突变型p53蛋白(mp53)的存在情况。该单克隆抗体对大多数哺乳动物的mp53具有特异性,但对野生型蛋白无特异性。在10例良性乳腺疾病患者中,只有2例(20%)血清中可检测到mp53水平。在乳腺癌组中,30例无淋巴结转移的患者中有7例(23%)血清mp53呈阳性,45例有转移性淋巴结的患者中有7例(15%)血清mp53呈阳性,7例有播散性疾病的患者中有1例(14%)血清mp53呈阳性。在20名健康对照者中评估的mp53检测特异性为100%。这些初步结果表明,血清mp53阳性与乳腺疾病的进展无关。目前正在进行进一步的研究,以评估mp53作为乳腺癌可能的预后因素的效用。
