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[Pt(HPxSC)Cl(3)],一种具有抗癌特性的新型铂(IV)化合物。

[Pt(HPxSC)Cl(3)], a novel platinum(IV) compound with anticancer properties.

作者信息

Marković Milos, Knezević Nikola, Momcilović Miljana, Grgurić-Sipka Sanja, Harhaji Ljubica, Trajković Vladimir, Mostarica Stojković Marija, Sabo Tibor, Miljković Djordje

机构信息

Institute of Microbiology and Immunology, School of Medicine, University of Belgrade, Dr. Subotica 1, 11000 Belgrade, Serbia and Montenegro.

出版信息

Eur J Pharmacol. 2005 Jul 4;517(1-2):28-34. doi: 10.1016/j.ejphar.2005.05.038.

DOI:10.1016/j.ejphar.2005.05.038
PMID:15970285
Abstract

There has been a continuing effort for the discovery of novel platinum(IV)-based antitumor compounds with better therapeutic performances than cisplatin. In the present work, the anticancer action of recently synthesized Pt(IV)-based complex [Pt(HPxSC)Cl(3)] was investigated using rat and human astrocytoma cell lines C6 and U251. [Pt(HPxSC)Cl(3)] markedly reduced the number of cultured astrocytoma cells (IC(50), 80 microM), as determined by crystal violet assay. The Pt(IV) complex induced apoptotic death of tumor cells, as flow cytometry analysis of the propidium iodide-stained cellular DNA revealed approx. 30% of hypodiploid cells in [Pt(HPxSC)Cl(3)]-treated astrocytoma cell cultures. On the other hand, [Pt(HPxSC)Cl(3)] at 200 microM did not affect the viability of rat primary astrocytes, unlike the established anticancer drug cisplatin, which displayed high toxicity toward both astrocytoma cells (IC(50), 15 microM) and primary astrocytes (IC(50), 20 microM). Moreover, [Pt(HPxSC)Cl(3)] at 100 microM did not interfere with the ability of rat peritoneal macrophages to produce important antitumor molecules nitric oxide and tumor necrosis factor-alpha. Finally, we assessed the ability of [Pt(HPxSC)Cl(3)] to restrain growth of some bacterial and yeast strains, but it showed rather limited antimicrobial activity.

摘要

人们一直在不断努力发现新型铂(IV)基抗肿瘤化合物,使其具有比顺铂更好的治疗性能。在本研究中,使用大鼠和人类星形细胞瘤细胞系C6和U251,研究了最近合成的铂(IV)基配合物[Pt(HPxSC)Cl(3)]的抗癌作用。通过结晶紫测定法确定,[Pt(HPxSC)Cl(3)]显著减少了培养的星形细胞瘤细胞数量(IC50,80微摩尔)。碘化丙啶染色细胞DNA的流式细胞术分析显示,铂(IV)配合物诱导肿瘤细胞凋亡死亡,在[Pt(HPxSC)Cl(3)]处理的星形细胞瘤细胞培养物中约有30%的亚二倍体细胞。另一方面,与已确立的抗癌药物顺铂不同,200微摩尔的[Pt(HPxSC)Cl(3)]不影响大鼠原代星形胶质细胞的活力,顺铂对星形细胞瘤细胞(IC50,15微摩尔)和原代星形胶质细胞(IC50,20微摩尔)均表现出高毒性。此外,100微摩尔的[Pt(HPxSC)Cl(3)]不干扰大鼠腹膜巨噬细胞产生重要抗肿瘤分子一氧化氮和肿瘤坏死因子-α的能力。最后,我们评估了[Pt(HPxSC)Cl(3)]抑制一些细菌和酵母菌株生长的能力,但它显示出相当有限的抗菌活性。

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