Olsen Pauline M, Ruiz Charles, Lussier Daniel, Le Brian Khoa, Angel Noah, Smith Michelle, Hwang Chihyun Brian, Khatib Raneen, Jenkins Julia, Adams Kaitlyn, Getcher Jonathan, Tham Fook, Chen Zhou Georgia, Wilson Emma H, Eichler Jack F
University of California, Riverside, Department of Chemistry, Riverside, CA 92521-0129, USA.
Emory University Winship Cancer Institute, Atlanta, GA, USA.
J Inorg Biochem. 2014 Dec;141:121-131. doi: 10.1016/j.jinorgbio.2014.08.014. Epub 2014 Sep 6.
Gold(III) complexes bearing bidentate ligands based on the 1,10-phenanthroline and 2,2'-bipyridine scaffolds have shown promising anticancer activity against a variety of tumor cell lines. In particular, our laboratory has previously found that a pseudo five coordinate gold(III) complex possessing the 2,9-di-sec-butyl-1,10-phenanthroline ligand {[((di-sec-butyl)phen)AuCl3]} exhibits antitumor activity against a panel of five different lung and head-neck tumor cell lines. However, the [((di-sec-butyl)phen)AuCl3] complex was determined to be less active than the free 2,9-di-sec-butyl-1,10-phenanthroline ligand. In order to determine if this class of gold(III) complexes has a distinct mechanism of initiating tumor cell death or if these gold complexes simply release the polypyridyl ligand in the intracellular environment, structural analogues of the [((di-sec-butyl)phen)AuCl3] complex have been synthesized and structurally characterized. These structural congeners were prepared by using mono-alkyl and di-phenyl substituted 1,10-phenanthroline ligands, di-alkyl and di-phenyl substituted 4-methyl-1,10-phenanthroline ligands, and mono-alkyl 2,2'-bipyridine ligands. The redox stability of this library of distorted square pyramidal gold(III) complexes has been studied and the in vitro antitumor activity of gold(III) complexes and corresponding polypyridyl ligands has been determined. The [((di-n-butyl)phen)AuCl3] and [((mono-n-butyl)phen)AuCl3] complexes have been found to be significantly more potent at inhibiting the growth of A549 lung tumor cells than the clinically used drug cisplatin. More importantly, these two gold(III) complexes are significantly more active than their respective free ligands, providing evidence that this class of pseudo five coordinate gold(III) complexes has a mechanism of initiating tumor cell death that is independent of the free ligand.
基于1,10 - 菲咯啉和2,2'-联吡啶骨架的含二齿配体的金(III)配合物,已显示出对多种肿瘤细胞系具有有前景的抗癌活性。特别是,我们实验室先前发现,一种具有2,9 - 二仲丁基 - 1,10 - 菲咯啉配体的准五配位金(III)配合物{[((二仲丁基)菲)AuCl3]}对一组五种不同的肺癌和头颈肿瘤细胞系具有抗肿瘤活性。然而,[((二仲丁基)菲)AuCl3]配合物被确定比游离的2,9 - 二仲丁基 - 1,10 - 菲咯啉配体活性更低。为了确定这类金(III)配合物引发肿瘤细胞死亡是否具有独特机制,或者这些金配合物是否只是在细胞内环境中释放多吡啶配体,已合成并对[((二仲丁基)菲)AuCl3]配合物的结构类似物进行了结构表征。这些结构类似物是通过使用单烷基和二苯基取代的1,10 - 菲咯啉配体、二烷基和二苯基取代的4 - 甲基 - 1,10 - 菲咯啉配体以及单烷基2,2'-联吡啶配体制备的。已研究了这个畸变四方锥金(III)配合物库的氧化还原稳定性,并测定了金(III)配合物和相应多吡啶配体的体外抗肿瘤活性。已发现[((二正丁基)菲)AuCl3]和[((单正丁基)菲)AuCl3]配合物在抑制A549肺癌细胞生长方面比临床使用的药物顺铂显著更有效。更重要的是,这两种金(III)配合物比它们各自的游离配体活性显著更高,这证明这类准五配位金(III)配合物具有一种独立于游离配体引发肿瘤细胞死亡的机制。
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