RELATIVE INVOLVEMENT OF PROTEIN-KINASE-C AND OF THE ESTROGEN-RECEPTOR IN THE CYTOTOXIC ACTION OF A POPULATION OF TRIPHENYLETHYLENES ON MCF(7) CELLS AS REVEALED BY CORRESPONDENCE FACTORIAL (CF) ANALYSIS

被引:10
作者
OJASOO, T
BIGNON, E
DEPAULET, AC
DORE, JC
GILBERT, J
MIQUEL, JF
PONS, M
RAYNAUD, JP
机构
[1] INSERM, U58, 60 RUE NAVACELLES, F-34090 MONTPELLIER, FRANCE
[2] ROUSSEL UCLAF, F-75007 PARIS, FRANCE
[3] MUSEUM NATL HIST NAT, CNRS, URA 401, F-75005 PARIS, FRANCE
[4] CNRS, CERCOA, F-94320 THIAIS, FRANCE
关键词
D O I
10.1016/0960-0760(93)90084-A
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
A multivariate statistical method, correspondence factorial (CF) analysis, was used to examine the correlations among the protein binding and cell proliferation effects of a series of 36 di- and triphenylethylenes (DPEs and TPEs). The analysis was applied to a study which measured their competition for estradiol binding to cytosol estrogen receptor (ER), their influence on protein kinase C (PKC) activity under different conditions of enzyme activation, their ability to promote the growth of a breast cancer cell line and to inhibit growth at high concentrations (cytotoxicity). The CF analysis revealed several levels of correlation. First, it distinguished those molecules within the population that stimulated rather than inhibited PKC activity. Second, it made apparent a strong correlation between cytotoxicity and inhibition of Ca++ and phosphatidylserine-dependent PKC activity, which was most marked when the enzyme had been activated by diacylglycerol indicating that PKC inhibition under physiological conditions might contribute to the overall cytotoxicity of these compounds. Third, a lower level of correlation was established between competition for ER binding and cytotoxicity. Taken together, the results suggest that MCF7 cells might be most sensitive to a cytotoxic effect of TPEs (via PKC and other targets) when they at the same time decrease estrogen-stimulated proliferation via an ER-mediated antiestrogenic effect.
引用
收藏
页码:239 / 250
页数:12
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