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设计、合成及雌二醇-聚乙二醇连接铂(II)杂化分子的生物学评价:三种不同结构类型杂化物的比较分子模拟研究。

Design, synthesis and biological evaluation of estradiol-PEG-linked platinum(II) hybrid molecules: comparative molecular modeling study of three distinct families of hybrids.

机构信息

Groupe de Recherche en Oncologie et Endocrinologie Moléculaires, Département de Chimie-Biologie, Université du Québec à Trois-Rivières, C.P. 500, Trois-Rivières, Québec, Canada.

出版信息

Steroids. 2011 Jan;76(1-2):94-103. doi: 10.1016/j.steroids.2010.09.004. Epub 2010 Oct 30.

DOI:10.1016/j.steroids.2010.09.004
PMID:20869376
Abstract

The synthesis of a series of 17β-estradiol-platinum(II) hybrid molecules is reported. The hybrids are made of a PEG linking chain of various length and a 2-(2'-aminoethyl)pyridine ligand. They are prepared from estrone in only 5 chemical steps with an overall yield of 22%. The length of the PEG chain does not influence the solubility of the compounds as it remains relatively constant throughout the series. MTT assays showed that the derivative with the longest PEG chain showed the best activity against two human breast cancer cell lines (MCF-7 and MDA-MB-231). The novel PEG-hybrids are also compared in terms of activities with two other families of 17β-estradiol-platinum(II) hybrids that we reported in previous studies. Molecular modeling study performed on a representative member of each family of hybrids reveals distinct molecular interactions with the estrogen receptor α which further corroborates their notably contrasting cytocidal activities on breast cancer cell lines. This study also shows that lipophilicity and the orientation of the tether chain between the estrogenic portion and the platinum(II) core contribute markedly to the biological activity of the various families of hybrids. The most active hybrids are those possessing an alkyl tether chain at position 16β of the steroid nucleus. For example, derivative 3 (p=6) is about 16 times more potent on MCF-7 breast cancer cells than the corresponding 16α-PEG-hybrids (2b) made in this study.

摘要

报道了一系列 17β-雌二醇-铂(II)杂化分子的合成。这些杂化物由不同长度的 PEG 连接链和 2-(2'-氨基乙基)吡啶配体组成。它们是由雌酮通过仅 5 步化学反应制备的,总收率为 22%。PEG 链的长度不影响化合物的溶解度,因为在整个系列中它保持相对恒定。MTT 测定表明,具有最长 PEG 链的衍生物对两种人乳腺癌细胞系(MCF-7 和 MDA-MB-231)表现出最好的活性。新型 PEG 杂化物还与我们在先前研究中报道的另外两种 17β-雌二醇-铂(II)杂化物家族进行了活性比较。对每种杂化物家族的代表性成员进行的分子建模研究揭示了与雌激素受体α的不同分子相互作用,这进一步证实了它们在乳腺癌细胞系上明显不同的细胞毒性活性。该研究还表明,亲脂性和亲核性部分与铂(II)核心之间的连接链的取向对各种杂化物家族的生物活性有显著贡献。最活跃的杂化物是那些在甾体核的 16β 位具有烷基连接链的杂化物。例如,衍生物 3(p=6)在 MCF-7 乳腺癌细胞上的活性比本研究中制备的相应 16α-PEG 杂化物(2b)高约 16 倍。

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