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首页> 外文期刊>European Journal of Medicinal Chemistry: Chimie Therapeutique >Synthesis, antiproliferative activity and estrogen receptor α affinity of novel estradiol-linked platinum(II) complex analogs to carboplatin and oxaliplatin. Potential vector complexes to target estrogen-dependent tissues.
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Synthesis, antiproliferative activity and estrogen receptor α affinity of novel estradiol-linked platinum(II) complex analogs to carboplatin and oxaliplatin. Potential vector complexes to target estrogen-dependent tissues.

机译:新型雌二醇连接的铂(II)配合物类似物对卡铂和奥沙利铂的合成,抗增殖活性和雌激素受体α亲和力。靶向雌激素依赖性组织的潜在载体复合物。

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In the course of efforts to develop 17β-estradiol-linked to anticancer agents targeting estrogen-dependent tissue, we identified three estradiol-linked platinum(II) complex analogs to cisplatin (E-CDDP) derivatives namely: VP-128 (1), CD-38 (2) and JMP-39 (3) that exhibit potent in?vitro and in?vivo (for derivative VP-128) activity along with interaction with the estrogen receptor α (ERα). In this study, we prepared and biologically evaluated two novel classes of estradiol-linked platinum(II) complex analogs to carboplatin (E-CarboP, 1a-3a) and oxaliplatin (E-OxaP, 1b-3b). E-CarboP and E-OxaP were designed and based on the estradiol-linker scaffold of E-CDDP derivatives previously identified. Consequently, we assessed the importance of the nature of platinum(II) salt on the antiproliferative activity on MCF-7 and MDA-MB-231 human mammary carcinoma cell lines together with affinity for the ERα by replacing the dichloroplatinum(II) moiety by a cyclobutane-1,1-dicarboxylateplatinum(II) or an oxalateplatinum(II) moiety. Except for compound 3b which is inactive at the concentration tested, the antiproliferative activity of all compounds on both human mammary carcinomas cell lines are in micromolar range and are more active than carboplatin and oxaliplatin alone but less active that their E-CDDP counterparts (1-3). In addition, E-CarboP derivatives 1a-3a show very low affinity for ERα whereas E-OxaPs 1b and 2b show higher affinity for ERα than their parents E-CDDPs (1-2), suggesting that the nature of the platinum(II) salt involved in the vector complexes is extremely important to both retain significant antiproliferative activity and selectivity for the ERα and possibility to target estrogen-dependent tissues. Finally, E-OxaPs 1b and 2b are potentially promising alternatives vector complexes to target estrogen-dependent tissues.
机译:在努力开发与靶向雌激素依赖性组织的抗癌药连接的17β-雌二醇的过程中,我们鉴定了三种与顺铂(E-CDDP)衍生物雌激素连接的铂(II)复合物类似物:VP-128(1), CD-38(2)和JMP-39(3)表现出强大的体外和体内活性(对于衍生物VP-128),并且与雌激素受体α(ERα)相互作用。在这项研究中,我们制备了两类与卡铂(E-CarboP,1a-3a)和奥沙利铂(E-OxaP,1b-3b)的雌二醇连接的铂(II)复合物类似物,并对其进行了生物学评估。 E-CarboP和E-OxaP的设计是基于先前鉴定的E-CDDP衍生物的雌二醇-连接骨架。因此,我们评估了铂盐(II)的性质对MCF-7和MDA-MB-231人乳癌细胞系抗增殖活性的重要性以及对ERα的亲和力,方法是用二氯铂(II)取代二氯铂(II)部分环丁烷-1,1-二羧酸铂(II)或草酸酯铂(II)部分。除了在测试浓度下没有活性的化合物3b以外,所有化合物对两种人类乳腺癌细胞系的抗增殖活性均在微摩尔范围内,并且比单独的卡铂和奥沙利铂具有更高的活性,但其活性却低于其E-CDDP对应物(1- 3)。此外,E-CarboP衍生物1a-3a对ERα的亲和力很低,而E-OxaPs 1b和2b对ERα的亲和力比其亲本E-CDDP高(1-2),这表明铂(II)的性质载体复合物中所含的盐对于保持显着的抗增殖活性和对ERα的选择性以及靶向雌激素依赖性组织的可能性非常重要。最后,E-OxaPs 1b和2b是靶向雌激素依赖性组织的潜在有前途的替代载体复合物。

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