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ZR-75-1人乳腺癌细胞变体中表皮生长因子受体和胰岛素样生长因子I受体的表达呈负相关:类固醇激素对胰岛素样生长因子I受体表达的影响。

Expression of receptors for epidermal growth factor and insulin-like growth factor I by ZR-75-1 human breast cancer cell variants is inversely related: the effect of steroid hormones on insulin-like growth factor I receptor expression.

作者信息

van den Berg H W, Claffie D, Boylan M, McKillen J, Lynch M, McKibben B

机构信息

Department of Therapeutics and Pharmacology, The Queen's University of Belfast, UK.

出版信息

Br J Cancer. 1996 Feb;73(4):477-81. doi: 10.1038/bjc.1996.84.

Abstract

We have investigated the expression of insulin-like growth factor I receptors (IGFR) by the ZR-75-1 human breast cancer cell line and tamoxifen-resistant (ZR-75-9a1) and oestrogen-independent (ZR-PR-LT) variants. ZR-75-1 cells expressed 6633+/-953 receptors per cell,(K(d) 0.24+/-0.06 nM). IGFR expression was reduced in ZR-75-9a1 cells (1180+/-614 receptors per cell, K(d) 0.13+/-0.05) and increased in the ZR-PR-LT cell line (18 430+/-3210 receptors per cell, K(d) 0.24+/-17). A comparison of these data with previously published findings for epidermal growth factor receptor (EGFR) expression by these cell lines revealed that IGFR and EGFR expression are inversely related in the variant lines whereas ZR-75-1 cells express similar numbers of both receptors. Since the changes in IGFR expression observed are associated with changes in steroid hormone receptor status, we also investigated the effects of oestradiol, the synthetic progestin ORG 2058 and dexamethasone on IGFR expression. Oestradiol increased IGFR expression only in the ZR-75-1 cell line. Low concentrations of ORG 2058 increased IGFR levels in the two cell lines positive for progesterone receptor (ZR-75-1 and ZR-PR-LT). High concentrations of ORG 2058 increased IGFR expression in all cell lines, as did dexamethasone. These data suggest that EGFR and IGFR expression may be linked in breast cancer, and that EGFR/IGFR ratios in breast cancer may be a more sensitive prognostic indicator than EGFR expression alone. Regardless of basal IGFR expression by the cell studied, ORG 2058 increased IGFR expression, possibly via both the progesterone and glucocorticoid receptors.

摘要

我们研究了ZR - 75 - 1人乳腺癌细胞系及其耐他莫昔芬(ZR - 75 - 9a1)和雌激素非依赖性(ZR - PR - LT)变体中胰岛素样生长因子I受体(IGFR)的表达情况。ZR - 75 - 1细胞每个细胞表达6633±953个受体,解离常数(K(d))为0.24±0.06 nM。IGFR表达在ZR - 75 - 9a1细胞中减少(每个细胞1180±614个受体,K(d) 0.13±0.05),而在ZR - PR - LT细胞系中增加(每个细胞18430±3210个受体,K(d) 0.24±0.17)。将这些数据与之前发表的关于这些细胞系表皮生长因子受体(EGFR)表达的研究结果进行比较发现,在变体细胞系中IGFR和EGFR表达呈负相关,而ZR - 75 - 1细胞表达的这两种受体数量相似。由于观察到的IGFR表达变化与类固醇激素受体状态的变化相关,我们还研究了雌二醇、合成孕激素ORG 2058和地塞米松对IGFR表达的影响。雌二醇仅在ZR - 75 - 1细胞系中增加IGFR表达。低浓度的ORG 2058增加了孕激素受体阳性的两个细胞系(ZR - 75 - 1和ZR - PR - LT)中的IGFR水平。高浓度的ORG 2058以及地塞米松在所有细胞系中均增加了IGFR表达。这些数据表明,EGFR和IGFR表达在乳腺癌中可能存在关联,并且乳腺癌中的EGFR/IGFR比值可能比单独的EGFR表达是更敏感的预后指标。无论所研究细胞的基础IGFR表达如何,ORG 2058可能通过孕激素和糖皮质激素受体两者增加IGFR表达。

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