在人乳腺癌模型中，纯甾体类抗雌激素与他莫昔芬的效果比较。

Comparison of the effects of a pure steroidal antiestrogen with those of tamoxifen in a model of human breast cancer.

作者信息

Osborne C K, Coronado-Heinsohn E B, Hilsenbeck S G, McCue B L, Wakeling A E, McClelland R A, Manning D L, Nicholson R I

机构信息

Department of Medicine, University of Texas Health Science Center at San Antonio 78284-7884, USA.

出版信息

J Natl Cancer Inst. 1995 May 17;87(10):746-50. doi: 10.1093/jnci/87.10.746.

DOI:10.1093/jnci/87.10.746

PMID:7563152

Abstract

BACKGROUND

Tamoxifen, a nonsteroidal estrogen antagonist, is the most prescribed drug for the treatment of breast cancer. The use of tamoxifen is limited, however, by the development of resistance to this compound in most patients. Although tamoxifen behaves primarily as an estrogen antagonist, it has agonist (or growth-stimulatory) activity as well. ICI 182,780 is a 7 alpha-alkylsulfinyl analogue of estradiol lacking agonist activity. The absence of agonist activity may make this steroidal antiestrogen superior to tamoxifen in suppressing tumor cell growth.

PURPOSE

We compared the inhibitory effects of ICI 182,780, tamoxifen, and estrogen withdrawal on the growth of established tumors and on tumorigenesis in a model system that uses estrogen-dependent, human MCF-7 breast tumor cells growing in athymic nude mice. We also studied the hormonal responsiveness of tumors that became resistant to the two estrogen antagonists and the effects of these drugs on estrogen-regulated gene expression.

METHODS

MCF-7 cells were injected subcutaneously into the flanks of castrated, female nude mice. The effects of repeated doses of tamoxifen and ICI 182,780 (500 micrograms and 5 mg, respectively) on the growth of established tumors (8-10 mm in size) were determined after supplemental estrogen was removed. The effects of antiestrogen treatments on the process of tumorigenesis, in the absence of estrogen supplementation, were determined by initiating drug administration on the same day as tumor cell inoculation. To evaluate the hormonal responsiveness of tumors resistant to tamoxifen and ICI 182,780, 1-mm3 segments of the tumors were transplanted onto the flanks of new recipient mice, which were then treated with estrogen or the antiestrogens--alone or in combination. Tumor growth was monitored by measuring tumor volumes twice a week. Expression of the estrogen-responsive genes, pLIV1 and pS2, in the tumors of treated animals was analyzed using blots of total cellular RNA and complementary DNA probes.

RESULTS

Treatment with ICI 182,780 suppressed the growth of established tumors twice as long as treatment with tamoxifen or estrogen withdrawal. Tumorigenesis, in the absence of supplemental estrogen, was delayed to a greater extent in ICI 182,780-treated mice than in tamoxifen-treated mice. ICI 182,780 was found to be more effective than tamoxifen in reducing the expression of estrogen-regulated genes. Most tumors eventually became resistant to ICI 182,780 and grew independently of estrogen.

CONCLUSIONS

ICI 182,780 is a more effective estrogen antagonist than tamoxifen in the MCF-7 tumor cell/nude mouse model system.

摘要

背景

他莫昔芬是一种非甾体类雌激素拮抗剂，是治疗乳腺癌最常用的药物。然而，大多数患者会对这种化合物产生耐药性，从而限制了他莫昔芬的使用。尽管他莫昔芬主要表现为雌激素拮抗剂，但它也具有激动剂（或生长刺激）活性。ICI 182,780是一种缺乏激动剂活性的雌二醇7α-烷基亚磺酰类似物。缺乏激动剂活性可能使这种甾体类抗雌激素在抑制肿瘤细胞生长方面优于他莫昔芬。

目的

我们在一个使用雌激素依赖性人MCF-7乳腺肿瘤细胞在无胸腺裸鼠体内生长的模型系统中，比较了ICI 182,780、他莫昔芬和雌激素撤除对已建立肿瘤生长和肿瘤发生的抑制作用。我们还研究了对这两种雌激素拮抗剂产生耐药性的肿瘤的激素反应性以及这些药物对雌激素调节基因表达的影响。

方法

将MCF-7细胞皮下注射到去势雌性裸鼠的侧腹。在去除补充雌激素后，确定重复剂量的他莫昔芬和ICI 182,780（分别为500微克和5毫克）对已建立肿瘤（大小为8 - 10毫米）生长的影响。在不补充雌激素的情况下，通过在肿瘤细胞接种当天开始给药来确定抗雌激素治疗对肿瘤发生过程的影响。为了评估对他莫昔芬和ICI 182,780产生耐药性的肿瘤的激素反应性，将1立方毫米的肿瘤组织移植到新的受体小鼠侧腹，然后用雌激素或抗雌激素单独或联合治疗。每周测量两次肿瘤体积以监测肿瘤生长。使用总细胞RNA印迹和互补DNA探针分析治疗动物肿瘤中雌激素反应基因pLIV1和pS2的表达。

结果

ICI 182,780治疗抑制已建立肿瘤生长的时间是他莫昔芬或雌激素撤除治疗的两倍。在不补充雌激素的情况下，ICI 182,780治疗的小鼠肿瘤发生延迟程度大于他莫昔芬治疗的小鼠。发现ICI 182,780在降低雌激素调节基因表达方面比他莫昔芬更有效。大多数肿瘤最终对ICI 182,780产生耐药性并独立于雌激素生长。