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乳腺癌的HER-2/neu基因分型在骨转移时可能会发生改变。

HER-2/neu genotype of breast cancer may change in bone metastasis.

作者信息

Lôrincz Tamás, Tóth József, Badalian Gayane, Tímár József, Szendrôi Miklós

机构信息

Department of Orthopedics, Semmelweis University, Budapest, Hungary.

出版信息

Pathol Oncol Res. 2006;12(3):149-52. doi: 10.1007/BF02893361. Epub 2006 Sep 23.

Abstract

The genotype of breast cancer (BRC) is considered to be relatively stable during tumor progression, accordingly, determination of the estrogen receptor and HER-2/neu status is currently based on the primary tumor. However, recent data suggest that the gene expression profile of the metastatic lesion can be different compared to that of the primary BRC. Accordingly, it is possible that the HER-2/neu status is different in the metastatic lesion and the primary BRC. Since the bone is the most frequent metastatic site during the progression of BRC, we have analyzed the HER-2/neu status of 48 bone metastatic BRC cases by immunohistochemistry and fluorescent in situ hybridization, and it was possible to compare it to the primary site in 23 cases. The frequency of HER-2/neu amplification of BRC in the primary tumors was found to be 17.4% compared to 10.5% in bone metastases. Half of BRC cases with HER-2/neu amplification lost this genotype in bone metastases (4/23 versus 2/23, respectively) and even in the 2 cases where HER-2/neu amplification was retained in the metastases, the copy number was found to be decreased compared to the primary tumor. Based on our data and previous reports in the literature, we suggest to perform HER-2/neu testing both on primary tumor and samples obtained from BRC metastases, at least in case of primary tumors with HER-2/neu amplification, before introduction of HER-2/neu-targeting therapy.

摘要

乳腺癌(BRC)的基因型在肿瘤进展过程中被认为相对稳定,因此,雌激素受体和HER-2/neu状态的测定目前基于原发性肿瘤。然而,最近的数据表明,与原发性BRC相比,转移病灶的基因表达谱可能有所不同。因此,转移病灶和原发性BRC的HER-2/neu状态有可能不同。由于骨是BRC进展过程中最常见的转移部位,我们通过免疫组织化学和荧光原位杂交分析了48例骨转移BRC病例的HER-2/neu状态,并且在23例病例中能够将其与原发部位进行比较。原发性肿瘤中BRC的HER-2/neu扩增频率为17.4%,而骨转移中为10.5%。HER-2/neu扩增的BRC病例中有一半在骨转移中失去了这种基因型(分别为4/23和2/23),甚至在转移灶中保留HER-2/neu扩增的2例病例中,与原发性肿瘤相比,拷贝数也减少了。基于我们的数据和文献中的先前报道,我们建议在引入HER-2/neu靶向治疗之前,至少对原发性肿瘤以及从BRC转移灶获取的样本进行HER-2/neu检测,尤其是对于原发性肿瘤有HER-2/neu扩增的情况。

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