THE DIRHENIUM(III) COMPLEX COMPOUNDS WITH IMIDAZOLE AND BENZIMIDAZOLE

O. Velychko, O. Golichenko, O. Shtemenko
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引用次数: 1

Abstract

Imidazole and it’s derivatives are structural fragments of certain enzymes, aminoacids, alkaloids and drugs. To date, the participation of imidazole in human metabolism, especially in the biosynthesis of natural purine bases of RNA and DNA, has been proven. Benzimidazole is one of the most used compound in medical chemistry. The various derivatives of substances, that exhibit analgesic, antidiabetic, anti-inflammatory, antitumor and antiviral activities were synthesized based on benzimidazole. This fact paves the way for the synthesis of antimetabolites, which can delay biosynthesis during biotransformation and inhibit the growth of malignant tumors. Thus, in the present work, the interaction of complex compounds with a single cluster fragment of Re 2 6+ (NBu 4 ) 2 Re 2 Cl 8 and trans-tetrachlorodi-μ-alkylcarboxylates of dirhenium(III) with representatives of the azole class – imidazole and benzimidazole was studied under various conditions. As a result of the experiments, methods for the synthesis of cis-[Re 2 (X) 4 Cl 4 (CH 3 CN) 2 ]Cl 2 (X is imidazole, benzimidazole) in an electron-donating organic solvent – CH3CN under heating in an inert atmosphere were developed. The starting materials were (NBu4)2Re2Cl8 and the selected azoles at a molar ratio of 1:10. The yield of the target compounds was 67-75%. We also investigated the reaction between trans-tetrachloridi-μ-alkylcarboxylates of dirhenium(III) and indicated azoles in a non-donor solvent (1,2-dichloroethane) in inert atmosphere at a molar ratio of reactants of 1:20. As a result of the interaction, complex compounds of the general formula (XH) 2 Re 2 Cl 8 (X – imidazole, benzimidazole) are formed, in which azoles are cations. The yield of reaction products was 83-87%. All target substances are synthesized, isolated in individual state, their spectral properties are investigated. The composition and structure of the obtained complex compounds were confirmed by IR- and NMR- spectroscopy on 1H and 13C, conductometry, and electronic absorption spectroscopy.
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与咪唑和苯并咪唑配合物的dihenium (iii)
咪唑及其衍生物是某些酶、氨基酸、生物碱和药物的结构片段。迄今为止,咪唑参与人体代谢,特别是RNA和DNA的天然嘌呤碱基的生物合成,已被证实。苯并咪唑是医学化学中应用最广泛的化合物之一。以苯并咪唑为基础合成了多种具有镇痛、降糖、抗炎、抗肿瘤和抗病毒活性的衍生物。这一事实为抗代谢产物的合成铺平了道路,抗代谢产物可以延缓生物转化过程中的生物合成,抑制恶性肿瘤的生长。因此,本研究在不同条件下,研究了含Re 2 6+ (NBu 4) 2 Re 2 Cl 8单簇片段和反四氯-μ-烷基羧酸diheni (III)的配合物与咪唑类代表物咪唑和苯并咪唑的相互作用。实验结果表明,在惰性气氛下,以供电子有机溶剂CH3CN为原料,在加热条件下合成顺式[Re 2 (X) 4 Cl 4 (CH3CN) 2]Cl 2 (X为咪唑,苯并咪唑)。原料为(NBu4)2Re2Cl8和所选的唑类化合物,摩尔比为1:10。目标化合物的收率为67 ~ 75%。我们还研究了在惰性气氛下,在非供体溶剂(1,2-二氯乙烷)中,在反应物摩尔比为1:20的条件下,反四氯-μ-烷基羧酸diheni (III)与指示唑的反应。由于相互作用的结果,形成了通式(XH) 2re2cl8 (X -咪唑,苯并咪唑)的络合物,其中唑是阳离子。反应产物收率为83 ~ 87%。合成并分离了所有的靶物质,并对其光谱性质进行了研究。通过1H、13C、IR、NMR、电导、电子吸收等方法对化合物的组成和结构进行了确证。
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