Human serum albumin as a copper source for anticancer thiosemicarbazones.

IF 2.9 3区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Metallomics Pub Date : 2023-08-01 DOI:10.1093/mtomcs/mfad046
Martin Schaier, Enrico Falcone, Tomas Prstek, Bertrand Vileno, Sonja Hager, Bernhard K Keppler, Petra Heffeter, Gunda Koellensperger, Peter Faller, Christian R Kowol
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引用次数: 0

Abstract

Thiosemicarbazones (TSCs) are a class of biologically active compounds with promising anticancer activity. Their typical mechanism, especially of the clinically far developed representative Triapine, is chelation of iron (Fe), with the Fe-containing enzyme ribonucleotide reductase as primary intracellular target. However, for the subclass of terminally disubstituted, nanomolar-active derivatives like Dp44mT and Me2NNMe2, recent findings suggest that the chelation, stability, and reduction properties of the copper(II) (Cu) complexes are essential for their modes of action. Consequently, it is important to elucidate whether blood serum Cu(II) is a potential metal source for these TSCs. To gain more insights, the interaction of Triapine, Dp44mT or Me2NNMe2 with purified human serum albumin (HSA) as the main pool of labile Cu(II) was investigated by UV-vis and electron paramagnetic resonance measurements. Subsequently, a size-exclusion chromatography inductively coupled plasma mass spectrometry method for the differentiation of Cu species in serum was developed, especially separating the non-labile Cu enzyme ceruloplasmin from HSA. The results indicate that the TSCs specifically chelate copper from the N-terminal Cu-binding site of HSA. Furthermore, the Cu(II)-TSC complexes were shown to form ternary HSA conjugates, most likely via histidine. Noteworthy, Fe-chelation from transferrin was not overserved, even not for Triapine. In summary, the labile Cu pool of HSA is a potential source for Cu-TSC complex formation and, consequently, distinctly influences the anticancer activity and pharmacological behavior of TSCs.

人血清白蛋白作为抗癌硫代氨基甲酸铜的铜源。
硫代氨基脲(TSCs)是一类生物活性化合物,具有良好的抗癌活性。它们的典型机理,尤其是临床上开发较早的代表药物 Triapine,是以含铁的核糖核苷酸还原酶为主要细胞内靶标,对铁(Fe)进行螯合。然而,对于 Dp44mT 和 Me2NNMe2 等亚类末端二取代、具有纳摩尔活性的衍生物,最近的研究结果表明,铜(II)(Cu)配合物的螯合、稳定性和还原特性对其作用模式至关重要。因此,阐明血清中的铜(II)是否是这些 TSCs 的潜在金属源非常重要。为了获得更深入的了解,我们通过紫外可见光和电子顺磁共振测量法研究了 Triapine、Dp44mT 或 Me2NNMe2 与纯化的人血清白蛋白(HSA)的相互作用。随后,研究人员开发了一种尺寸排阻色谱电感耦合等离子体质谱法,用于区分血清中的铜物种,特别是将非易化铜酶脑磷脂从 HSA 中分离出来。结果表明,TSCs 能从 HSA 的 N 端铜结合位点特异性地螯合铜。此外,Cu(II)-TSC 复合物很可能通过组氨酸形成三元 HSA 共轭物。值得注意的是,转铁蛋白中的铁螯合作用并没有被过度保留,甚至对 Triapine 也没有。总之,HSA 的易变 Cu 池是 Cu-TSC 复合物形成的潜在来源,因此会明显影响 TSCs 的抗癌活性和药理作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Metallomics
Metallomics 生物-生化与分子生物学
CiteScore
7.00
自引率
5.90%
发文量
87
审稿时长
1 months
期刊介绍: Global approaches to metals in the biosciences
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