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镉对人乳腺癌细胞中雌激素受体水平及雌激素诱导反应的影响。

Effect of cadmium on estrogen receptor levels and estrogen-induced responses in human breast cancer cells.

作者信息

Garcia-Morales P, Saceda M, Kenney N, Kim N, Salomon D S, Gottardis M M, Solomon H B, Sholler P F, Jordan V C, Martin M B

机构信息

Department of Biochemistry and Molecular Biology, Vincent T. Lombardi Cancer Research Center, Georgetown University, Washington, D.C. 20007.

出版信息

J Biol Chem. 1994 Jun 17;269(24):16896-901.

PMID:8207012
Abstract

The effects of cadmium on estrogen receptor and other estrogen-regulated genes in the human breast cancer cell line MCF-7 were studied. Treatment of MCF-7 cells with 1 microM cadmium decreased the level of estrogen receptor 58%. Cadmium induced a parallel decrease in estrogen receptor mRNA (62%). Progesterone receptor levels increased 3.2-fold after cadmium treatment. This induction was blocked by the anti-estrogen ICI-164,384. Progesterone receptor mRNA was also increased by cadmium, as well as cathepsin D mRNA. An in vitro nuclear transcription run-on assay showed that cadmium increased the transcription of the progesterone receptor and pS2 genes and decreased transcription of the estrogen receptor gene. These are not general effects of heavy metals, as zinc, 25 and 100 microM, did not affect progesterone receptor protein and mRNA levels. Cadmium stimulated pS2 and progesterone receptor mRNAs in a clone of MDA-MB-231 cells transfected with the human estrogen receptor, but had no effect in MDA-MB-231 cells transfected with antisense estrogen receptor. Cadmium also stimulated an estrogen response element in transient transfection experiments. These data suggest that the effects of cadmium are mediated by the estrogen receptor independent of estradiol. In addition to its effect on gene expression, cadmium induced the growth of MCF-7 cells 5.6-fold.

摘要

研究了镉对人乳腺癌细胞系MCF - 7中雌激素受体及其他雌激素调节基因的影响。用1微摩尔镉处理MCF - 7细胞后,雌激素受体水平降低了58%。镉使雌激素受体mRNA水平平行下降(62%)。镉处理后孕酮受体水平增加了3.2倍。这种诱导作用被抗雌激素ICI - 164,384阻断。镉还使孕酮受体mRNA以及组织蛋白酶D mRNA增加。体外细胞核转录连续分析表明,镉增加了孕酮受体和pS2基因的转录,降低了雌激素受体基因的转录。这并非重金属的普遍作用,因为25微摩尔和100微摩尔的锌并未影响孕酮受体蛋白和mRNA水平。镉刺激了转染人雌激素受体的MDA - MB - 231细胞克隆中的pS2和孕酮受体mRNA,但对转染反义雌激素受体的MDA - MB - 231细胞没有影响。在瞬时转染实验中,镉还刺激了雌激素反应元件。这些数据表明,镉的作用是由雌激素受体介导的,与雌二醇无关。除了对基因表达的影响外,镉使MCF - 7细胞的生长增加了5.6倍。

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