Ciocca Daniel R, Gago Francisco E, Fanelli Mariel A, Calderwood Stuart K
Laboratory of Oncology, Institute of Experimental Medicine and Biology of Cuyo (IMBECU-CONICET), Casilla de Correo 855, 5500 Mendoza, Argentina.
J Steroid Biochem Mol Biol. 2006 Dec;102(1-5):32-40. doi: 10.1016/j.jsbmb.2006.09.008. Epub 2006 Oct 17.
The response of breast cancer patients to endocrine therapy is guided by the expression of two steroid hormone receptors (HR): estrogen receptor alpha (ERalpha) and/or progesterone receptors (PR). In most laboratories the expression of these predictive markers is studied by immunohistochemistry (IHC) in the breast cancer biopsy samples. Another molecular marker that is being increasingly examined in breast cancer is the oncoprotein Her-2/neu, whose expression/amplification predicts the response to anti-Her-2/neu immunotherapy. The co-expression of HR with that of Her-2/neu is infrequent (most reports agree on this), however, there are some conflicting reports about the clinical implications in term of response to endocrine therapy in the patients that co-express HR and Her-2/neu. We have examined these molecular markers for a number of years in our tumor bank, in this dissertation we will present the method and cut-off to study these markers, the correlations between their expression, and the follow-up of the patients that received tamoxifen-based endocrine therapy, alone or following chemotherapy. We confirmed that the co-expression of HR with Her-2/neu is infrequent, and that these patients presented both a shorter disease free survival and overall survival. Our results will be compared with others related recently published. For example, the aromatase inhibitor anastrozole appears to be an effective endocrine treatment in HR+ patients, irrespective of the Her-2/neu status. We will present data on the molecular mechanisms that could explain the relatively poor outcome of these patients. Heregulin has been found to be a potent inducer of heat shock factor 1 (HSF1) activity and of heat shock protein (Hsp) synthesis in breast cancer cells and HSF1 activation plays a role in the tumorigenic changes induced by heregulin, heregulin exerts its tumorigenic changes through the cell surface tyrosine kinase receptors c-erbB-3 and c-erbB-4 which are able to form dimers with the "ligandless" Her-2/neu. We found that HSF1 associates with metastasis associated protein 1 (MTA1) on the promoters of genes as well as other molecules involved in gene repression (HDAC1, HDAC2) in a manner that is enhanced by either heregulin exposure or heat shock. ERs, although promoting the growth of breast cancer cells are less associated with invasion/metastasis and ER-induced gene expression is involve in this effect. Heregulin can overcome the protective effects of ER and at least a component of this appears to be due to MTA1 repression of ERE dependent transcription, HSF1 and MTA1 cooperate in gene repression. The co-expression of HSF1 and MTA1 was confirmed by IHC in human breast cancer biopsy samples.
乳腺癌患者对内分泌治疗的反应由两种类固醇激素受体(HR)的表达来指导:雌激素受体α(ERα)和/或孕激素受体(PR)。在大多数实验室中,这些预测标志物的表达是通过免疫组织化学(IHC)在乳腺癌活检样本中进行研究的。另一种在乳腺癌中越来越受到关注的分子标志物是癌蛋白Her-2/neu,其表达/扩增可预测对抗Her-2/neu免疫治疗的反应。HR与Her-2/neu的共表达并不常见(大多数报道对此观点一致),然而,对于共表达HR和Her-2/neu的患者,其对内分泌治疗反应的临床意义存在一些相互矛盾的报道。多年来,我们一直在肿瘤库中检测这些分子标志物,在本论文中,我们将介绍研究这些标志物的方法和临界值、它们表达之间的相关性,以及接受他莫昔芬内分泌治疗(单独或化疗后)患者的随访情况。我们证实HR与Her-2/neu的共表达并不常见,并且这些患者的无病生存期和总生存期均较短。我们的结果将与近期发表的其他相关结果进行比较。例如,芳香化酶抑制剂阿那曲唑似乎是HR+患者有效的内分泌治疗药物,与Her-2/neu状态无关。我们将展示可能解释这些患者相对较差预后的分子机制的数据。在这里发现,Heregulin是乳腺癌细胞中热休克因子1(HSF1)活性和热休克蛋白(Hsp)合成的有效诱导剂,HSF1激活在Heregulin诱导的致瘤性变化中起作用,Heregulin通过细胞表面酪氨酸激酶受体c-erbB-3和c-erbB-4发挥其致瘤性变化,这两种受体能够与“无配体”的Her-2/neu形成二聚体。我们发现HSF1与基因启动子上的转移相关蛋白1(MTA1)以及其他参与基因抑制的分子(HDAC1、HDAC2)相关联,这种关联在Heregulin暴露或热休克时会增强。ER虽然促进乳腺癌细胞的生长,但与侵袭/转移的关联较小,ER诱导的基因表达参与了这一效应。Heregulin可以克服ER的保护作用,至少部分原因似乎是MTA1对ERE依赖性转录的抑制,HSF-1和MTA1在基因抑制中协同作用。通过免疫组化在人乳腺癌活检样本中证实了HSF1和MTA1的共表达。
