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抗糖尿病钒配合物在全血及其成分中的反应性和形态:红细胞的重要作用

Reactivity and Speciation of Anti-Diabetic Vanadium Complexes in Whole Blood and Its Components: The Important Role of Red Blood Cells.

作者信息

Levina Aviva, McLeod Andrew I, Gasparini Sylvia J, Nguyen Annie, De Silva W G Manori, Aitken Jade B, Harris Hugh H, Glover Chris, Johannessen Bernt, Lay Peter A

机构信息

†School of Chemistry, The University of Sydney, Sydney NSW 2006, Australia.

‡Australian Synchrotron, 800 Blackburn Rd., Clayton VIC 3168, Australia.

出版信息

Inorg Chem. 2015 Aug 17;54(16):7753-66. doi: 10.1021/acs.inorgchem.5b00665. Epub 2015 Jul 31.

Abstract

Reactions with blood components are crucial for controlling the antidiabetic, anticancer, and other biological activities of V(V) and V(IV) complexes. Despite extensive studies of V(V) and V(IV) reactions with the major blood proteins (albumin and transferrin), reactions with whole blood and red blood cells (RBC) have been studied rarely. A detailed speciation study of Na3[V(V)O4] (A), K4[V(IV)2O2(citr)2]·6H2O (B; citr = citrato(4-)); [V(IV)O(ma)2] (C; ma = maltolato(-)), and (NH4)[V(V)(O)2(dipic)] (D; dipic = pyridine-2,6-dicarboxylato(2-)) in whole rat blood, freshly isolated rat plasma, and commercial bovine serum using X-ray absorption near-edge structure (XANES) spectroscopy is reported. The latter two compounds are potential oral antidiabetic drugs, and the former two are likely to represent their typical decomposition products in gastrointestinal media. XANES spectral speciation was performed by principal component analysis and multiple linear regression techniques, and the distribution of V between RBC and plasma fractions was measured by electrothermal atomic absorption spectroscopy. Reactions of A, C, or D with whole blood (1.0 mM V, 1-6 h at 310 K) led to accumulation of ∼50% of total V in the RBC fraction (∼10% in the case of B), which indicated that RBC act as V carriers to peripheral organs. The spectra of V products in RBC were independent of the initial V complex, and were best fitted by a combination of V(IV)-carbohydrate (2-hydroxyacid moieties) and/or citrate (65-85%) and V(V)-protein (15-35%) models. The presence of RBC created a more reducing environment in the plasma fraction of whole blood compared with those in isolated plasma or serum, as shown by the differences in distribution of V(IV) and V(V) species in the reaction products of A-D in these media. At physiologically relevant V concentrations (<50 μM), this role of RBC may promote the formation of V(III)-transferrin as a major V carrier in the blood plasma. The results reported herein have broad implications for the roles of RBC in the transport and speciation of metal pro-drugs that have broad applications across medicine.

摘要

与血液成分的反应对于控制V(V)和V(IV)配合物的抗糖尿病、抗癌及其他生物活性至关重要。尽管对V(V)和V(IV)与主要血液蛋白(白蛋白和转铁蛋白)的反应进行了广泛研究,但与全血和红细胞(RBC)的反应却鲜有研究。本文报道了利用X射线吸收近边结构(XANES)光谱对Na3[V(V)O4](A)、K4[V(IV)2O2(citr)2]·6H2O(B;citr = 柠檬酸根(4-))、[V(IV)O(ma)2](C;ma = 麦芽醇根(-))和(NH4)[V(V)(O)2(dipic)](D;dipic = 吡啶-2,6-二羧酸根(2-))在大鼠全血、新鲜分离的大鼠血浆和市售牛血清中的详细形态分析。后两种化合物是潜在的口服抗糖尿病药物,前两种可能代表它们在胃肠道介质中的典型分解产物。通过主成分分析和多元线性回归技术进行XANES光谱形态分析,并用电热原子吸收光谱法测定V在RBC和血浆部分之间的分布。A、C或D与全血(1.0 mM V,310 K下1 - 6小时)的反应导致约50%的总V积累在RBC部分(B的情况下约为10%),这表明RBC作为V载体将其转运至外周器官。RBC中V产物的光谱与初始V配合物无关,并且通过V(IV)-碳水化合物(2-羟基酸部分)和/或柠檬酸盐(65 - 85%)以及V(V)-蛋白质(15 - 35%)模型的组合能得到最佳拟合。与分离的血浆或血清相比,RBC的存在使全血血浆部分的环境更具还原性,则A - D在这些介质中的反应产物中V(IV)和V(V)物种的分布差异表明了这一点。在生理相关的V浓度(<50 μM)下,RBC的这种作用可能促进血浆中主要V载体V(III)-转铁蛋白的形成。本文报道的结果对于RBC在金属前药的运输和形态形成中的作用具有广泛影响,这些金属前药在医学上有广泛应用。

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