Comparative Solution Equilibrium Studies on Anticancer Estradiol-Based Conjugates and Their Copper Complexes

IF 3.1 4区 化学 Q2 CHEMISTRY, INORGANIC & NUCLEAR Inorganics Pub Date : 2024-02-01 DOI:10.3390/inorganics12020049
É. A. Enyedy, Anett Giricz, Tatsiana V. Petrasheuskaya, J. Mészáros, N. May, Gabriella Spengler, F. Kovács, Barnabás Molnár, Éva Frank
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Abstract

Steroids are often considered valuable molecular tools for the development of anticancer agents with improved pharmacological properties. Conjugation of metal chelating moieties with a lipophilic sterane backbone is a viable option to obtain novel anticancer compounds. In this work, two estradiol-based hybrid molecules (PMA-E2 and DMA-E2) with an (N,N,O) binding motif and their Cu(II) complexes were developed. The lipophilicity, solubility, and acid-base properties of the novel ligands were determined by the combined use of UV-visible spectrophotometry, pH-potentiometry, and 1H NMR spectroscopy. The solution speciation and redox activity of the Cu(II) complexes were also investigated by means of UV-visible and electron paramagnetic resonance spectroscopy. Two structurally analogous ligands (PMAP and DMAP) were also included in the studies for better interpretation of the solution chemical data obtained. Three pKa values were determined for all ligands, revealing the order of the deprotonation steps: pyridinium-NH+ or NH(CH3)2+, secondary NH2+, and OH. The dimethylamine derivatives (DMA-E2, DMAP) are found in their H2L+ forms in solution at pH 7.4, whereas the fraction of the neutral HL species is significant (34–37%) in the case of the pyridine nitrogen-containing derivatives (PMA-E2, PMAP). Both estradiol derivatives were moderately cytotoxic in human breast (MCF-7) and colon adenocarcinoma (Colo-205) cells (IC50 = 30–63 μM). They form highly stable complexes with Cu(II) ions capable of oxidizing ascorbate and glutathione. These Cu(II) complexes are somewhat more cytotoxic (IC50 = 15–45 μM) than their corresponding ligands and show a better selectivity profile.
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基于抗癌雌二醇的共轭物及其铜配合物的溶液平衡对比研究
类固醇通常被认为是开发具有更好药理特性的抗癌剂的重要分子工具。将金属螯合分子与亲脂性甾烷骨架共轭是获得新型抗癌化合物的一种可行方法。在这项研究中,我们开发了两种以雌二醇为基础、具有(N,N,O)结合基团的混合分子(PMA-E2 和 DMA-E2)及其铜(II)配合物。通过紫外-可见分光光度法、pH-电位法和 1H NMR 光谱法测定了新型配体的亲脂性、溶解性和酸碱特性。此外,还通过紫外可见光谱和电子顺磁共振光谱研究了 Cu(II) 复合物的溶液标示和氧化还原活性。为了更好地解释所获得的溶液化学数据,研究中还加入了两种结构类似的配体(PMAP 和 DMAP)。为所有配体测定了三个 pKa 值,揭示了去质子化步骤的顺序:吡啶鎓-NH+ 或 NH(CH3)2+、仲NH2+ 和羟基。在 pH 值为 7.4 的溶液中,二甲基胺衍生物(DMA-E2、DMAP)以 H2L+ 的形式存在,而在含吡啶氮衍生物(PMA-E2、PMAP)中,中性 HL 物种的比例很大(34-37%)。这两种雌二醇衍生物在人类乳腺癌(MCF-7)和结肠腺癌(Colo-205)细胞中都具有中度细胞毒性(IC50 = 30-63 μM)。它们与能够氧化抗坏血酸和谷胱甘肽的 Cu(II) 离子形成高度稳定的复合物。这些 Cu(II) 复合物的细胞毒性(IC50 = 15-45 μM)略高于相应的配体,并显示出更好的选择性。
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来源期刊
Inorganics
Inorganics Chemistry-Inorganic Chemistry
CiteScore
2.80
自引率
10.30%
发文量
193
审稿时长
6 weeks
期刊介绍: Inorganics is an open access journal that covers all aspects of inorganic chemistry research. Topics include but are not limited to: synthesis and characterization of inorganic compounds, complexes and materials structure and bonding in inorganic molecular and solid state compounds spectroscopic, magnetic, physical and chemical properties of inorganic compounds chemical reactivity, physical properties and applications of inorganic compounds and materials mechanisms of inorganic reactions organometallic compounds inorganic cluster chemistry heterogenous and homogeneous catalytic reactions promoted by inorganic compounds thermodynamics and kinetics of significant new and known inorganic compounds supramolecular systems and coordination polymers bio-inorganic chemistry and applications of inorganic compounds in biological systems and medicine environmental and sustainable energy applications of inorganic compounds and materials MD
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