Antiproliferative and receptor binding properties of alpha- and beta-casomorphins in the T47D human breast cancer cell line

被引:48
|
作者
Hatzoglou, A [1 ]
Bakogeorgou, E [1 ]
Hatzoglou, C [1 ]
Martin, PM [1 ]
Castanas, E [1 ]
机构
[1] CJF 9311 INSERM, EXPT CANCEROL LAB, MARSEILLE, FRANCE
关键词
alpha-casomorphin; beta-casomorphin; opioid receptor; receptor subtype; somatostastin receptor; breast cancer cell; T47D;
D O I
10.1016/0014-2999(96)00339-1
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
In previous studies, we have shown that opioid agonists ([D-Ala(2),D-Leu(5)]enkephalin (DADLE), [D-Ser(2),Leu(5)]enkephalin-Thr(6) (DSLET), ethylketocyclazocine and etorphine) bind to opioid binding sites and decrease cell proliferation of human T47D breast cancer cells. Furthermore, we provided evidence about a cross-reaction, also in the T47D human breast cancer cell line, of mu-acting opioids with type-II somatostatin receptors. Since a potential source of opioid activity in the breast might be casomorphin peptides (produced by the enzymatic degradation of alpha-casein and beta-casein), we investigated the antiproliferative action of five different casomorphin peptides: alpha-casein-(90-95), alpha-casein-(90-96), beta-casomorphin, beta-casomorphin-(1-5) and morphiceptin. We show that all five peptides decreased, in a dose-dependent manner, cell proliferation. The general antagonist diprenorphine produced only a partial reversal of their action. Furthermore, we provide evidence that all peptides (except for morphiceptin) bind to delta- and kappa-opioid binding sites of T47D cells with different selectivity. Finally, we show that these peptides are also partial competitors at the somatostatin receptors present in the same cell line.
引用
收藏
页码:217 / 223
页数:7
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