首页> 外文期刊>Journal of Inorganic Biochemistry: An Interdisciplinary Journal >Reactivity of potential anti-diabetic molybdenum(VI) complexes in biological media: a XANES spectroscopic study
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Reactivity of potential anti-diabetic molybdenum(VI) complexes in biological media: a XANES spectroscopic study

机译:生物介质中潜在抗糖尿病钼(VI)配合物的反应性:XANES光谱研究

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The application of Mo(VI) complexes as anti-diabetic agents is a subject of considerable recent interest. The stability and speciation of [Mo(VI)O(4)](2-) and three analogs of known anti-diabetic V(IV) complexes ([Mo(VI)O(2)L(2)]; where LH=2,4-pentanedione, l-cysteine ethyl ester or N,N-diethyldithiocarbamic acid) in natural and simulated biological fluids (including blood and its components, cell culture media, and artificial digestion systems) were studied using MoK-edge XANES (X-ray absorption near-edge structure) spectroscopy of freeze-dried samples at 20K. All of the studied [MoO(2)L(2)] complexes decomposed extensively under simulated gastric and intestinal digestion conditions (3 h at 310 K), as well as in blood plasma or in cell culture medium (24 h at 310 K). The reaction products of [MoO(4)](2-) and [MoO(2)L(2)] with biological fluids could be satisfactorily modelled (using multiple linear regression analyses) as mixtures of tetrahedral and octahedral Mo(VI) species (with O-donor ligands) in various ratios, which were dependent on the nature of the medium rather than that of the initial Mo(VI) compounds. Red blood cells take up Mo(VI) predominantly in the form of [MoO(4)](2-). Implications of these results to the development of Mo(VI)-based anti-diabetics and to the mechanisms of natural uptake and metabolism of Mo(VI) are discussed.
机译:Mo(VI)配合物作为抗糖尿病药的应用是近期引起广泛关注的主题。 [Mo(VI)O(4)](2-)和已知抗糖尿病V(IV)配合物([Mo(VI)O(2)L(2)]的三个类似物的稳定性和形态使用MoK-edge XANES研究了自然和模拟生物流体(包括血液及其成分,细胞培养基和人工消化系统)中的= 2,4-戊二酮,L-半胱氨酸乙酯或N,N-二乙基二硫代氨基甲酸。 X射线吸收近边缘结构)在20K下冷冻干燥的样品的光谱。所有研究的[MoO(2)L(2)]复合物在模拟的胃和肠消化条件下(310 K下3 h),以及血浆或细胞培养基(310 K下24 h)广泛分解。 。 [MoO(4)](2-)和[MoO(2)L(2)]与生物流体的反应产物可以令人满意地建模(使用多重线性回归分析),为四面体和八面体Mo(VI)的混合物(具有O-供体配体)的各种比率,取决于介质的性质,而不是初始Mo(VI)化合物的性质。红细胞主要以[MoO(4)](2-)的形式吸收Mo(VI)。讨论了这些结果对基于Mo(VI)的抗糖尿病药的开发以及对Mo(VI)天然摄取和代谢机制的影响。

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