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首页> 外文期刊>Bioinorganic chemistry and applications >Reversible Dissociation and Ligand-Glutathione Exchange Reaction in Binuclear Cationic Tetranitrosyl Iron Complex with Penicillamine
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Reversible Dissociation and Ligand-Glutathione Exchange Reaction in Binuclear Cationic Tetranitrosyl Iron Complex with Penicillamine

机译:双核阳离子四亚硝基铁与青霉素胺的可逆离解和配体-谷胱甘肽交换反应

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摘要

This paper describes a comparative study of the decomposition of two nitrosyl iron complexes (NICs) with penicillamine thiolic ligands [Fe2(SC5H11NO2)2(NO)4]SO4·5H2O (I) and glutathione- (GSH-) ligands [Fe2(SC10H17N3O6)2(NO)4]SO4·2H2O (II), which spontaneously evolve to NO in aqueous medium. NO formation was measured by a sensor electrode and by spectrophotometric methods by measuring the formation of a hemoglobin- (Hb-) NO complex. The NO evolution reaction rate from (I)  k1= (4.6 ± 0.1)·10−3 s−1and the elimination rate constant of the penicillamine ligandk2= (1.8 ± 0.2)·10−3 s−1at 25°C in 0.05 M phosphate buffer,  pH 7.0, was calculated using kinetic modeling based on the experimental data. Both reactions are reversible. Spectrophotometry and mass-spectrometry methods have firmly shown that the penicillamine ligand is exchanged for GS−during decomposition of 1.5·10−4 M (I) in the presence of 10−3 M GSH, with 76% yield in 24 h. As has been established, such behaviour is caused by the resistance of (II) to decomposition due to the higher affinity of iron to GSH in the complex. The discovered reaction may impede S-glutathionylation of the essential enzyme systems in the presence of (I) and is important for metabolism of NIC, connected with its antitumor activity.
机译:本文描述了两种带有青霉胺硫醇配体[Fe2(SC5H11NO2)2(NO)4] SO4·5H2O(I)和谷胱甘肽-(GSH-)配体[Fe2(SC10H17N3O6)的亚硝基铁络合物(NIC)分解的比较研究。 )2(NO)4] SO4·2H2O(II)在水性介质中自发生成NO。通过传感器电极和通过分光光度法通过测量血红蛋白-(Hb-)NO络合物的形成来测量NO的形成。 (I)k1 =(4.6±0.1)·10-3−s-1的NO释放反应速率和青霉素胺配体的消除速率常数k2 =(1.8±0.2)·10-3 s-1于25°C在0.05 M根据实验数据,使用动力学模型计算了磷酸盐缓冲液的pH值7.0。两种反应都是可逆的。分光光度法和质谱法已明确表明,在存在10−3 M GSH的情况下,在1.5·10−4 M(I)分解过程中,青霉素胺配体被GS-交换,在24 h内收率为76%。如已经确定的,这种行为是由于铁对配合物中GSH的较高亲和力而导致的(II)对分解的抗性引起的。发现的反应可能会在(I)存在的情况下阻碍必需酶系统的S-谷胱甘肽化,这对于NIC的代谢及其抗肿瘤活性至关重要。

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