氨基酸与铜的络合:l-谷氨酰胺-铜(II) - l-组氨酸三元体系

P. Deschamps, N. Zerrouk, T. Martens, M. Charlot, J. Girerd, J. Chaumeil, A. Tomáš
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引用次数: 6

摘要

门克斯病是一种致死性铜转运遗传性疾病。目前的治疗方法是使用铜- l-组氨酸复合物。然而,这种疗法只在某些情况下有效,并且在生命早期开始。由于铜(II)混合配体氨基酸配合物在生理铜途径中发挥重要作用,因此为了开发一种改进的处理方法,对铜(II)混合配体氨基酸配合物进行了研究。一个有前途的策略是给予l-组氨酸-铜(II) - l-谷氨酰胺复合物,据报道这是人类血清中主要的低分子量铜(II)复合物。在对l-组氨酸-铜(II) - l-谷氨酰胺络合物进行生物制药研究之前,必须对该三元体系进行物理化学研究。在pH为7的条件下,用极谱法和紫外可见光谱法测定了l-组氨酸-铜(II) - l-谷氨酰胺相对于铜(II) - l-组氨酸和铜(II) - l-谷氨酰胺的化学计量学和稳定性。然而,已经证明了[Cu(His)2]和[Cu(His)2(OH)]在同一溶液中共存。EPR分析表明[Cu(His)(Gln)]配合物中的铜具有扭曲的八面体几何形状。铜配位的第一层是3n, 1o,组氨酸和谷氨酸是双齿的。
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Copper Complexation by Amino Acid: l-Glutamine–Copper(II)–l-Histidine Ternary System
Abstract Menkes disease is a lethal genetic disorder of copper transport in humans. Its current treatment is the administration of copper–l-histidine complex. However, this therapy is only effective in some cases and when started early in life. In order to develop an improved treatment, copper(II) mixed ligand amino acid complexes were studied because these complexes play an important role in the physiological copper pathway. A promising strategy is the administration of l-histidine–copper(II)–l-glutamine complex, which has been reported to be the predominant low molecular-weight copper(II) complex in human blood serum. Before the biopharmaceutical studies of l-histidine–copper(II)–l-glutamine complex, a physicochemical study of this ternary system must be performed. The stoichiometry and the stability of l-histidine–copper(II)–l-glutamine relative to copper(II)–l-histidine and copper(II)–l-glutamine were established at pH 7 in solution by polarography and UV–visible spectroscopy. Nevertheless, it has been demonstrated that the species [Cu(His)2] and [Cu(His)2(OH)] coexist in the same solution. This study has been complemented by EPR analysis which suggests copper in [Cu(His)(Gln)] complex has a distorted octahedral geometry. The first shell of copper coordination is 3 N, 1 O, histidine, and glutarnine being bidentate.
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