JOURNAL ARTICLE

Copper Complexation by Amino Acid:l-Glutamine–Copper(II)–l-Histidine Ternary System

Abstract

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.

Keywords:
Copper Histidine Chemistry Glutamine Electron paramagnetic resonance Ternary operation Amino acid Ternary complex Ligand (biochemistry) Inorganic chemistry Biochemistry Organic chemistry Receptor Enzyme

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Citation History

Topics

Trace Elements in Health
Health Sciences →  Nursing →  Nutrition and Dietetics
Metal complexes synthesis and properties
Health Sciences →  Medicine →  Oncology
Drug Transport and Resistance Mechanisms
Health Sciences →  Medicine →  Oncology

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