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MDM2蛋白表达是乳腺癌的一个负性预后标志物。

MDM2 protein expression is a negative prognostic marker in breast carcinoma.

作者信息

Turbin Dmitry A, Cheang Maggie C U, Bajdik Chris D, Gelmon Karen A, Yorida Erika, De Luca Alessandro, Nielsen Torsten O, Huntsman David G, Gilks C Blake

机构信息

Genetic Pathology Evaluation Centre of the Department of Pathology, British Columbia Cancer Agency and University of British Columbia, Vancouver, BC, Canada.

出版信息

Mod Pathol. 2006 Jan;19(1):69-74. doi: 10.1038/modpathol.3800484.

Abstract

The protein encoded by the MDM2 oncogene inhibits the function of p53, leading to increased cell growth, avoidance of apoptosis, tolerance of genetic instability, and resistance to chemotherapy. The present study was performed to evaluate the relationship between MDM2 protein expression and survival in breast carcinoma. Two series of cases were used in this study: the first to identify the cutoff to be used in the interpretation of MDM2 immunostaining and perform preliminary survival analysis, and a second, independent series, to validate the findings from the first series and to perform multivariate analysis. For both series, archival sections of tissue microarrays were stained with anti-MDM2 antibody (NeoMarkers, Fremont, CA, USA) and MDM2 staining intensity was scored semiquantitatively. In the first series, 49 of 362 (14%) interpretable cases were positive for MDM2 expression, with 35 (10%) showing weak positivity and 14 (4%) strong positivity. Patients with MDM2-positive tumours had a significantly worse disease-specific survival than patients with MDM2-negative tumours (P=0.0022, 10-year DSS 61% (95% CI: 45-73) vs 73% (95% CI: 67-77)). No significant difference in survival was observed between patients with strongly and weakly MDM2-positive tumours (P=0.3). Accordingly, in the independent validation series weak and strong MDM2 positivity were combined and considered to be MDM2 positive. MDM2 expression was seen in 230/1747 (13%) interpretable cases in this series, with a significant difference (P<0.0001) in DSS between MDM2-negative and MDM2-positive cases (10 year DSS 58% (95% CI: 51-64) vs 73% (95% CI: 70-75)). MDM2 was an independent prognostic marker (HR=1.35, P=0.02) in a Cox regression model including MDM2 expression, tumour grade, nodal status, ER status and tumour size. Immunohistochemical studies of MDM2 in more than 2000 breast carcinomas show that MDM2 is an independent negative prognostic marker.

摘要

MDM2癌基因编码的蛋白质会抑制p53的功能,导致细胞生长增加、逃避凋亡、耐受基因不稳定并产生化疗耐药性。本研究旨在评估MDM2蛋白表达与乳腺癌患者生存率之间的关系。本研究使用了两个系列的病例:第一个系列用于确定MDM2免疫染色结果解读时的临界值并进行初步生存分析,第二个独立系列用于验证第一个系列的结果并进行多变量分析。对于这两个系列,组织微阵列的存档切片均用抗MDM2抗体(NeoMarkers,美国加利福尼亚州弗里蒙特)染色,并对MDM2染色强度进行半定量评分。在第一个系列中,362例可解读病例中有49例(14%)MDM2表达呈阳性,其中35例(10%)为弱阳性,14例(4%)为强阳性。MDM2阳性肿瘤患者的疾病特异性生存率显著低于MDM2阴性肿瘤患者(P=0.0022,10年疾病特异性生存率分别为61%(95%可信区间:45-73)和73%(95%可信区间:67-77))。MDM2强阳性和弱阳性肿瘤患者的生存率无显著差异(P=0.3)。因此,在独立验证系列中,将MDM2弱阳性和强阳性合并并视为MDM2阳性。该系列1747例可解读病例中有230例(13%)出现MDM2表达,MDM2阴性和阳性病例的疾病特异性生存率存在显著差异(P<0.0001)(10年疾病特异性生存率分别为58%(95%可信区间:51-64)和73%(95%可信区间:70-75))。在包含MDM2表达、肿瘤分级、淋巴结状态、雌激素受体状态和肿瘤大小的Cox回归模型中,MDM2是一个独立的预后标志物(风险比=1.35,P=0.02)。对2000多例乳腺癌进行的MDM2免疫组织化学研究表明,MDM2是一个独立的阴性预后标志物。

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