Buglyó Péter, Crans Debbie C, Nagy Eszter M, Lindo Ruby Lisa, Yang Luqin, Smee Jason J, Jin Wenzheng, Chi Lai-Har, Godzala Iii Michael E, Willsky Gail R
Department of Inorganic and Analytical Chemistry, University of Debrecen, P.O. Box 21, H-4010 Debrecen, Hungary.
Inorg Chem. 2005 Jul 25;44(15):5416-27. doi: 10.1021/ic048331q.
The aqueous vanadium(III) (V(III)) speciation chemistry of two dipicolinate-type complexes and the insulin-enhancing effects of V-dipicolinate (V-dipic) complexes in three different oxidation states (V(III), V(IV), and V(V)) have been studied in a chronic animal model system. The characterization of the V(III) species was carried out at low ionic strength to reflect physiological conditions and required an evaluation of the hydrolysis of V(III) at 0.20 M KCl. The aqueous V(III)-dipic and V(III)-dipic-OH systems were characterized, and complexes were observed from pH 2 to 7 at 0.2 M KCl. The V(III)-dipic system forms stable 1:2 complexes, whereas the V(III)-dipic-OH system forms stable 1:1 complexes. A comparison of these complexes with the V-pic system demonstrates that a second ligand has lower affinity for the V(III), presumably reflecting bidentate coordination of the second dipic(2)(-) to the V(III). The thermodynamic stability of the V(III)(dipic)(2) complex was compared to the stability of the corresponding V(IV) and V(V) complexes, and surprisingly, the V(III) complexes were found to be more stable than anticipated. Oral administration of three V-dipicolinate compounds in different oxidation states {H[V(III)(dipic)(2)H(2)O].3H(2)O, [V(IV)Odipic(H(2)O)(2)].2H(2)O, and NH(4)[V(V)O(2)dipic]} and the positive control, VOSO(4), significantly lowered diabetic hyperglycemia in rats with streptozotocin-induced diabetes. The diabetic animals treated with the V(III)- or V(IV)-dipic complexes had blood glucose levels that were statistically different from those of the diabetic group. The animals treated with the V(V)-dipic complex had the lowest blood glucose levels of the treated diabetic animals, which were statistically different from those of the diabetic group at all time points. Among the diabetic animals, complexation to dipic increased the serum levels of V after the administration of the V(V) and V(IV) complexes but not after the administration of the V(III) complex when data are normalized to the ingested dose of V. Because V compounds differing only in oxidation state have different biological properties, it is implied that redox processes must be important factors for the biological action of V compounds. We observe that the V(V)-dipic complex is the most effective insulin-enhancing agent, in contrast to previous studies in which the V(IV)-maltol complex is the most effective. We conclude that the effectiveness of complexed V is both ligand and oxidation state dependent.
在慢性动物模型系统中,研究了两种吡啶二甲酸酯类配合物的水相钒(III)(V(III))物种形成化学以及三种不同氧化态(V(III)、V(IV)和V(V))的钒-吡啶二甲酸酯(V-二吡啶)配合物的胰岛素增强作用。在低离子强度下对V(III)物种进行表征以反映生理条件,这需要评估0.20 M KCl条件下V(III)的水解情况。对水相V(III)-二吡啶和V(III)-二吡啶-OH体系进行了表征,在0.2 M KCl条件下,从pH 2到7观察到了配合物。V(III)-二吡啶体系形成稳定的1:2配合物,而V(III)-二吡啶-OH体系形成稳定的1:1配合物。将这些配合物与V-吡啶体系进行比较表明,第二个配体对V(III)的亲和力较低,这大概反映了第二个二吡啶(2)(-)与V(III)的双齿配位。将[V(III)(二吡啶)(2)](-)配合物的热力学稳定性与相应的V(IV)和V(V)配合物的稳定性进行了比较,令人惊讶的是,发现V(III)配合物比预期更稳定。口服三种不同氧化态的钒-吡啶二甲酸酯化合物{H[V(III)(二吡啶)(2)H(2)O].3H(2)O、[V(IV)O二吡啶(H(2)O)(2)].2H(2)O和NH(4)[V(V)O(2)二吡啶]}以及阳性对照VOSO(4),可显著降低链脲佐菌素诱导糖尿病大鼠的糖尿病高血糖水平。用V(III)-或V(IV)-二吡啶配合物治疗的糖尿病动物的血糖水平与糖尿病组有统计学差异。用V(V)-二吡啶配合物治疗的动物在所有治疗的糖尿病动物中血糖水平最低,在所有时间点与糖尿病组有统计学差异。在糖尿病动物中,当数据根据摄入的钒剂量进行归一化时,与二吡啶络合会增加V(V)和V(IV)配合物给药后血清中的钒水平,但V(III)配合物给药后则不会。由于仅氧化态不同的钒化合物具有不同的生物学特性,这意味着氧化还原过程必定是钒化合物生物学作用的重要因素。我们观察到,与之前研究中V(IV)-麦芽醇配合物最有效的情况相反,V(V)-二吡啶配合物是最有效的胰岛素增强剂。我们得出结论,络合钒的有效性既取决于配体也取决于氧化态。
