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通过多参数流式细胞术检测人乳腺癌中p53、Her-2/neu和ras过表达与非整倍体之间的相关性:浸润性导管癌中共同表型进化模式的证据

Correlations among p53, Her-2/neu, and ras overexpression and aneuploidy by multiparameter flow cytometry in human breast cancer: evidence for a common phenotypic evolutionary pattern in infiltrating ductal carcinomas.

作者信息

Smith C A, Pollice A A, Gu L P, Brown K A, Singh S G, Janocko L E, Johnson R, Julian T, Hyams D, Wolmark N, Sweeney L, Silverman J F, Shackney S E

机构信息

Department of Human Oncology, Allegheny University of the Health Sciences, Allegheny General Hospital, Pittsburgh, Pennsylvania 15212, USA.

出版信息

Clin Cancer Res. 2000 Jan;6(1):112-26.

Abstract

Human solid tumors develop multiple genetic abnormalities that accumulate progressively in individual cells during the course of tumor evolution. We sought to determine whether there are specific sequences of occurrence of these progressive evolutionary changes in human breast cancers by performing correlated cell-by-cell measurements of cell DNA content, p53 protein, Her-2/neu protein, and ras protein by multiparameter flow cytometry in 56 primary tumor samples obtained at surgery. In addition, p53 allelic loss and Her-2/neu gene amplification were determined by fluorescence in situ hybridization in cells from the same samples. We reasoned that if there is a specific order in which genetic changes occur, the same early changes would be found consistently in the cells with the fewest abnormalities. We reasoned further that late-developing abnormalities would not occur alone in individual cells but would almost always be found together with the early changes inherited by the same cells. By these criteria, abnormalities involving p53 generally occurred early in the course of development of invasive breast cancers, whereas ras protein overexpression was found to be a late-occurring phenomenon. Within individual tumors, cellular p53 overexpression was often observed alone in individual cells, whereas ras protein overexpression was rarely observed in the absence of p53 overexpression and/or Her-2/neu overexpression in the same cells. Furthermore, the intracellular level of each abnormally expressed protein was found to increase progressively as new abnormalities were acquired. Infiltrating ductal carcinomas exhibited characteristic phenotypic patterns in which p53 allelic loss and/or p53 protein overexpression, Her-2/neu amplification and/or overexpression, aneuploidy, and ras overexpression accumulated within individual cells. However, this pattern was not a prominent feature of lobular breast cancers. All six lobular breast cancers studied were diploid. p53 allelic loss and/or early p53 overexpression, and late ras cooverexpression in the same cells were less common in lobular breast cancers than in infiltrating ductal carcinomas. Although Her-21neu overexpression was a common finding in lobular breast cancers, Her-2/neu amplification was not observed in these tumors.

摘要

人类实体瘤会出现多种基因异常,这些异常在肿瘤进化过程中会在单个细胞中逐渐累积。我们试图通过多参数流式细胞术对56例手术切除的原发性肿瘤样本进行细胞DNA含量、p53蛋白、Her-2/neu蛋白和ras蛋白的逐细胞相关测量,来确定人类乳腺癌中这些渐进性进化变化的发生是否存在特定顺序。此外,通过荧光原位杂交确定同一样本细胞中的p53等位基因缺失和Her-2/neu基因扩增情况。我们推断,如果基因变化存在特定顺序,那么在异常最少的细胞中会一致地发现相同的早期变化。我们进一步推断,后期出现的异常不会单独出现在单个细胞中,而几乎总是会与同一细胞继承的早期变化同时出现。根据这些标准,涉及p53的异常通常发生在浸润性乳腺癌发展过程的早期,而ras蛋白过表达是后期出现的现象。在单个肿瘤内,经常在单个细胞中单独观察到细胞p53过表达,而在同一细胞中,在没有p53过表达和/或Her-2/neu过表达的情况下,很少观察到ras蛋白过表达。此外,随着新异常的出现,每种异常表达蛋白的细胞内水平逐渐升高。浸润性导管癌表现出特征性的表型模式,其中p53等位基因缺失和/或p53蛋白过表达、Her-2/neu扩增和/或过表达、非整倍体以及ras过表达在单个细胞中累积。然而,这种模式并非小叶性乳腺癌的显著特征。所研究的6例小叶性乳腺癌均为二倍体。与浸润性导管癌相比,小叶性乳腺癌中同一细胞内p53等位基因缺失和/或早期p53过表达以及后期ras共过表达的情况较少见。虽然Her-2/neu过表达在小叶性乳腺癌中很常见,但在这些肿瘤中未观察到Her-2/neu扩增。

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