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人表皮生长因子受体2(Her-2)过表达会增加乳腺癌细胞在脑内的转移生长。

Her-2 overexpression increases the metastatic outgrowth of breast cancer cells in the brain.

作者信息

Palmieri Diane, Bronder Julie L, Herring Jeanne M, Yoneda Toshiyuki, Weil Robert J, Stark Andreas M, Kurek Raffael, Vega-Valle Eleazar, Feigenbaum Lionel, Halverson Douglas, Vortmeyer Alexander O, Steinberg Seth M, Aldape Kenneth, Steeg Patricia S

机构信息

Laboratory of Molecular Pharmacology, Women's Cancers Section, National Cancer Institute, NIH, Bethesda, Maryland 20892, USA.

出版信息

Cancer Res. 2007 May 1;67(9):4190-8. doi: 10.1158/0008-5472.CAN-06-3316.

Abstract

Retrospective studies of breast cancer patients suggest that primary tumor Her-2 overexpression or trastuzumab therapy is associated with a devastating complication: the development of central nervous system (brain) metastases. Herein, we present Her-2 expression trends from resected human brain metastases and data from an experimental brain metastasis assay, both indicative of a functional contribution of Her-2 to brain metastatic colonization. Of 124 archival resected brain metastases from breast cancer patients, 36.2% overexpressed Her-2, indicating an enrichment in the frequency of tumor Her-2 overexpression at this metastatic site. Using quantitative real-time PCR of laser capture microdissected epithelial cells, Her-2 and epidermal growth factor receptor (EGFR) mRNA levels in a cohort of 12 frozen brain metastases were increased up to 5- and 9-fold, respectively, over those of Her-2-amplified primary tumors. Co-overexpression of Her-2 and EGFR was also observed in a subset of brain metastases. We then tested the hypothesis that overexpression of Her-2 increases the colonization of breast cancer cells in the brain in vivo. A subclone of MDA-MB-231 human breast carcinoma cells that selectively metastasizes to brain (231-BR) overexpressed EGFR; 231-BR cells were transfected with low (4- to 8-fold) or high (22- to 28-fold) levels of Her-2. In vivo, in a model of brain metastasis, low or high Her-2-overexpressing 231-BR clones produced comparable numbers of micrometastases in the brain as control transfectants; however, the Her-2 transfectants yielded 3-fold greater large metastases (>50 microm(2); P < 0.001). Our data indicate that Her-2 overexpression increases the outgrowth of metastatic tumor cells in the brain in this model system.

摘要

对乳腺癌患者的回顾性研究表明,原发性肿瘤Her-2过表达或曲妥珠单抗治疗与一种严重的并发症相关:中枢神经系统(脑)转移的发生。在此,我们展示了来自切除的人脑转移瘤的Her-2表达趋势以及来自实验性脑转移分析的数据,两者均表明Her-2对脑转移定植有功能性作用。在124例来自乳腺癌患者的存档切除脑转移瘤中,36.2%过表达Her-2,表明该转移部位肿瘤Her-2过表达频率有所富集。通过对激光捕获显微切割的上皮细胞进行定量实时PCR,12例冷冻脑转移瘤队列中Her-2和表皮生长因子受体(EGFR)的mRNA水平分别比Her-2扩增的原发性肿瘤高5倍和9倍。在一部分脑转移瘤中还观察到Her-2和EGFR的共过表达。然后我们检验了Her-2过表达会增加乳腺癌细胞在脑内定植的假说。选择性转移至脑的MDA-MB-231人乳腺癌细胞亚克隆(231-BR)过表达EGFR;用低水平(4至8倍)或高水平(22至28倍)的Her-2转染231-BR细胞。在体内脑转移模型中,低水平或高水平Her-2过表达的231-BR克隆在脑内产生的微转移灶数量与对照转染细胞相当;然而,Her-2转染细胞产生的大转移灶(>50平方微米;P<0.001)是对照的3倍。我们的数据表明,在该模型系统中,Her-2过表达会增加脑内转移瘤细胞的生长。

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