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大鼠中抗糖尿病钒吡啶甲酸酯配合物的结构依赖性金属动力学:溶液结构、胰岛素模拟活性和金属动力学研究

Structure-dependent metallokinetics of antidiabetic vanadyl-picolinate complexes in rats: studies on solution structure, insulinomimetic activity, and metallokinetics.

作者信息

Yasui Hiroyuki, Tamura Asuka, Takino Toshikazu, Sakurai Hiromu

机构信息

Department of Analytical and Bioinorganic Chemistry, Kyoto Pharmaceutical University, 5 Nakauchi-cho, Misasagi, Yamashina-ku, Kyoto 607-8414, Japan.

出版信息

J Inorg Biochem. 2002 Jul 25;91(1):327-38. doi: 10.1016/s0162-0134(02)00443-9.

Abstract

The insulinomimetic effect of vanadium is the most remarkable and important among its several biological actions. Vanadyl ion (+4 oxidation state of vanadium) and its complexes have been found to normalize the blood glucose levels of both type 1 and 2 diabetic animals. We have developed insulinomimetic vanadyl complexes having different coordination modes, emphasizing the possible usefulness of vanadyl-picolinate [VO(pa)(2)] and its related complexes with the VO(N(2)O(2)) coordination mode. In order to apply these complexes clinically in the future, the relationship between the chemical structure, insulinomimetic action, organ distribution of vanadium, and blood disposition of vanadyl species must be closely investigated. In the present investigation, we studied the blood disposition of the vanadyl-picolinate complexes in healthy rats, and tried to understand comprehensively the relationship between the structures, insulinomimetic activity, and metallokinetic parameters of the complexes, which had been recently prepared and specifically synthesized for the present study, by using an in vivo blood circulation monitoring -- electron spin resonance (BCM-ESR) method for analyzing ESR signals due to paramagnetic metal ions and complexes in the blood in real time. Metallokinetic parameters were estimated based on the blood clearance curves in terms of a two-compartment pharmacokinetic model, and vanadyl species were indicated to be distributed in peripheral tissues and gradually eliminated from the circulating blood, depending on their chemical structures. Vanadyl concentrations in the blood of rats given bis(5-iodopicolinato)oxovanadium(IV) [VO(5ipa)(2)] and bis(3-methylpicolinato)oxovanadium(IV) [VO(3mpa)(2)] with electron-withdrawing and donating groups, respectively, remained significantly higher and longer, due to their slower clearance rates from the blood, than in rats given other complexes, suggesting that the high exposure and long residence of vanadyl species bring about the high normoglyceric effect in diabetic animals. We then examined the relationship between insulinomimetic activity and metallokinetic parameters in the family of VO(pa)(2) for further development of insulinomimetic vanadyl complexes. IC(50), the 50% inhibitory concentration of the complexes on the free fatty acid release from isolated rat adipocytes treated with epinephrine, was found to be sufficiently correlated with metallokinetic parameters such as area under the concentration curve, mean residence time, total clearance, and distribution volume at steady-state. Furthermore, the in vivo antidiabetic activity of the complexes was enhanced with increasing exposure and residence of vanadyl species in the blood of animals. On the basis of these results, we concluded that in vitro insulinomimetic activity, metallokinetic character, and in vivo antidiabetic action of vanadyl-picolinate complexes are closely related to their chemical structures.

摘要

钒的拟胰岛素作用在其多种生物学作用中最为显著和重要。已发现钒离子(钒的+4氧化态)及其配合物可使1型和2型糖尿病动物的血糖水平恢复正常。我们已开发出具有不同配位模式的拟胰岛素钒配合物,重点研究了吡啶甲酸钒[VO(pa)(2)]及其具有VO(N(2)O(2))配位模式的相关配合物的潜在用途。为了将来将这些配合物应用于临床,必须深入研究钒的化学结构、拟胰岛素作用、器官分布以及钒基物种的血液处置之间的关系。在本研究中,我们研究了吡啶甲酸钒配合物在健康大鼠体内的血液处置情况,并试图通过使用体内血液循环监测——电子自旋共振(BCM-ESR)方法实时分析血液中顺磁性金属离子和配合物产生的ESR信号,全面了解最近为本研究专门制备和合成的配合物的结构、拟胰岛素活性和金属动力学参数之间的关系。基于二室药代动力学模型,根据血液清除曲线估算金属动力学参数,结果表明钒基物种根据其化学结构分布在外周组织中,并逐渐从循环血液中清除。分别给予具有吸电子基团和供电子基团的双(5-碘吡啶甲酸根)氧钒(IV)[VO(5ipa)(2)]和双(3-甲基吡啶甲酸根)氧钒(IV)[VO(3mpa)(2)]的大鼠血液中的钒浓度,由于其从血液中的清除速率较慢,显著高于且持续时间长于给予其他配合物的大鼠,这表明钒基物种的高暴露和长时间停留会在糖尿病动物中产生高降血糖作用。然后,我们研究了VO(pa)(2)家族中拟胰岛素活性与金属动力学参数之间的关系,以进一步开发拟胰岛素钒配合物。发现配合物对肾上腺素处理的离体大鼠脂肪细胞游离脂肪酸释放的50%抑制浓度IC(50)与浓度曲线下面积、平均停留时间、总清除率和稳态分布容积等金属动力学参数充分相关。此外,随着钒基物种在动物血液中的暴露和停留时间增加,配合物的体内抗糖尿病活性增强。基于这些结果,我们得出结论,吡啶甲酸钒配合物的体外拟胰岛素活性、金属动力学特征和体内抗糖尿病作用与其化学结构密切相关。

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