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Inhibition of acid, alkaline, and tyrosine (PTP1B) phosphatases by novel vanadium complexes

机译:新型钒配合物对酸性,碱性和酪氨酸(PTP1B)磷酸酶的抑制作用

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In the course of our investigations of vanadium-containing complexes for use as insulin-enhancing agents, we have generated a series of novel vanadium coordination complexes with bidentate ligands. Specifically we have focused on two ligands: anthranilate (anc(-)), a natural metabolite of tryptophan, and imidizole-4-carboxylate (imc(-)), meant to mimic naturally occurring N-donor ligands. For each ligand, we have generated a series of complexes containing the V(III), V(IV), and V(V) oxidation states. Each complex was investigated using phosphatase inhibition studies of three different phosphatases (acid, alkaline, and tyrosine (PTP1B) phosphatase) as prima facia evidence for potential use as an insulin-enhancing agent. Using p-nitrophenyl phosphate as an artificial phosphatase substrate, the levels of inhibition were determined by measuring the absorbance of the product at 405 nm using UV/vis spectroscopy. Under our experimental conditions, for instance, V(imc)(3) appears to be as potent an inhibitor of alkaline phosphatase as sodium orthovanaclate when comparing the K-cat/K-m term. VO(anc)(2) is as potent an inhibitor of acid phosphatase and tyrosine phosphatase as the Na3VO4. Thus, use of these complexes can increase our mechanistic understanding of the effects of vanadium in vivo.
机译:在我们研究用作胰岛素增强剂的含钒复合物的过程中,我们已经生成了一系列具有双齿配体的新型钒配位复合物。具体来说,我们专注于两个配体:邻氨基苯甲酸酯(anc(-)),一种色氨酸的天然代谢产物;和咪唑-4-羧酸酯(imc(-)),用于模拟天然存在的N供体配体。对于每个配体,我们生成了一系列包含V(III),V(IV)和V(V)氧化态的配合物。使用三种不同磷酸酶(酸,碱性和酪氨酸(PTP1B)磷酸酶)作为表面筋膜的磷酸酶抑制研究来研究每种复合物,以作为潜在的胰岛素增强剂。使用对硝基苯基磷酸酯作为人工磷酸酶底物,通过使用紫外/可见光谱法测量产物在405 nm的吸光度来确定抑制水平。例如,在我们的实验条件下,当比较K-cat / K-m项时,V(imc)(3)与原戊酸钠一样似乎是碱性磷酸酶的有效抑制剂。 VO(anc)(2)是与Na3VO4一样有效的酸性磷酸酶和酪氨酸磷酸酶抑制剂。因此,使用这些配合物可以增加我们对体内钒作用的机械理解。

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