Iodide n,π-chelate complexes of platinum(II) based on N-allyl substituted thioureas and their effect on the activity of hepatobiliary system enzymes in comparison with chloride analogs

V. Orysyk, L. Garmanchuk, S. Orysyk, Yu. L. Zborovskii, S. Shishkina, I. Stupak, P. Novikova, D. Ostapchenko, N. Khranovska, V. Pekhnyo, M. Vovk
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Abstract

The search for new effective drugs in the treatment of neoplasm remains relevant even today, since the adaptation of transformed cells to the action of classical drugs contributes to the emergence of drug resistance­. This applies to a number of classic chemotherapy drugs of the platinum series, in particular cisplatin. In this work, we describe the effect of novel analogs of cisplatin on HepG2 cells and on the key enzyme of antioxidant protection system gammaglutamyltranspeptidase, which plays an important role in the acquisition of drug resistance to anticancer drugs by tumor cells. New mononuclear iodide n,π-chelate complexes of Pt(II) with substituted thioureas N-allylmorpholine-4-carbothioamide or 3-allyl-1,1-diethylthiourea were obtained as analogs of cisplatin. All compounds were investigated by UV-Vis, IR, and 1H/13С NMR spectra. Complex I was described by single-crystal X-ray diffraction study. Also, the effect of these analogs on alanine aminotransferase, aspartate aminotransferase, lactate dehydrogenase, which are marker enzymes of liver cells, release of which into the blood indicates liver pathologies, was investigated. All studies were carried out in comparison with chloride n,π-chelate complexes of platinum obtained earlier (however, the effect of these chloride analogs of platinum on enzymes of the hepatobiliary system was investigated for the first time in this work). The results have shown that the studied compounds are better cytostatics/cytotoxics than cisplatin both according to IC50 and apoptosis level of HepG2 cells. It is established that, for the most part, effect of the studied complexes is reduced to a decrease in the degree of malignancy of cells of hepatocyte lines and the activity of LDH and GHT, as well as a decrease in consumed glucose. Keywords: alanine aminotransferase, aspartate aminotransferase, gammaglutamyltranspeptidase, lactate dehydrogenase, NMR spectroscopy, n‚π-chelates, thioureas
基于 N-烯丙基取代的硫脲类的铂(II)的 n,π-螯合碘化物配合物及其与氯化物类似物相比对肝胆系统酶活性的影响
由于转化细胞对传统药物作用的适应性导致了抗药性的出现,因此,寻找治疗肿瘤的新有效药物的工作至今仍具有现实意义。这适用于铂系列的一些经典化疗药物,尤其是顺铂。在这项工作中,我们描述了顺铂的新型类似物对 HepG2 细胞和抗氧化保护系统的关键酶伽玛谷氨酰转肽酶的影响,该酶在肿瘤细胞获得抗癌药物耐药性的过程中发挥着重要作用。研究人员获得了铂(II)与取代硫脲类化合物 N-烯丙基吗啉-4-硫代甲酰胺或 3-烯丙基-1,1-二乙基硫脲的新型单核碘化物 n,π-螯合物,作为顺铂的类似物。所有化合物均通过紫外可见光谱、红外光谱和 1H/13С NMR 光谱进行了研究。通过单晶 X 射线衍射研究对复合物 I 进行了描述。此外,还研究了这些类似物对丙氨酸氨基转移酶、天门冬氨酸氨基转移酶和乳酸脱氢酶的影响,丙氨酸氨基转移酶、天门冬氨酸氨基转移酶和乳酸脱氢酶是肝细胞的标志酶,释放到血液中表明肝脏出现病变。所有研究都是在与早先获得的氯化 n,π-螯合铂络合物进行比较的基础上进行的(不过,在这项工作中,首次研究了这些氯化铂类似物对肝胆系统酶的影响)。研究结果表明,根据 IC50 和 HepG2 细胞凋亡水平,所研究的化合物比顺铂具有更好的细胞抑制/细胞毒性。研究结果表明,所研究复合物的大部分作用是降低肝细胞系细胞的恶性程度、降低 LDH 和 GHT 的活性,以及降低消耗的葡萄糖。关键词:丙氨酸氨基转移酶、天冬氨酸氨基转移酶、甘谷氨酰转肽酶、乳酸脱氢酶、核磁共振光谱、n'π-螯合物、硫脲类化合物
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