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由铜(II)的混合配体配合物诱导的转铁蛋白铁释放

Iron release from transferrin induced by mixed ligand complexes of copper(II).

作者信息

Glaus M, Schneider W

机构信息

Laboratorium für anorganische Chemie, ETH-Zentrum, Zürich, Switzerland.

出版信息

Biol Met. 1989;2(3):185-90. doi: 10.1007/BF01142558.

Abstract

Copper(II) complexes CuL1L2 with the ligand pairs 3-phosphoglycerate (PG)/ethylenediamine (en), phosphoserine (PS)/ethylenediamine, phosphoserine/malonate (mal) are shown to be effective in inducing the release of both iron atoms from di-ferric transferrin (Fe2Tf; human serum transferrin) at pH 7.3 in 1 M NaCl at 25 degrees C. Half-times of the reaction with Cu(PG)(en)- were less than 1 min at 0.02 M concentration. The iron(III) products are polynuclear hydroxo complexes. There is weaker interaction with Cu(PS)4-2 and virtually none with Cu(serine)(en) nor Cu(PS)(2,2'-bipyridyl)-, revealing crucial effects of the combined ligand sphere including the phosphomonoester group. The results suggest that the release of iron from Fe2Tf, or from either monoferric transferrins, occurred due to the breakdown of the stability of iron binding in conjunction with the expulsion of the synergistic anion carbonate (or oxalate). The active copper(II) complexes are postulated to be models of membrane components that could liberate iron from transferrin succeeding its uptake at the receptor sites of cells.

摘要

已表明铜(II)配合物CuL1L2与配体对3-磷酸甘油酸(PG)/乙二胺(en)、磷酸丝氨酸(PS)/乙二胺、磷酸丝氨酸/丙二酸(mal)在25℃、pH 7.3的1 M NaCl溶液中能有效诱导二价铁转铁蛋白(Fe2Tf;人血清转铁蛋白)释放两个铁原子。在0.02 M浓度下,与Cu(PG)(en)-反应的半衰期小于1分钟。铁(III)产物是多核羟基配合物。与Cu(PS)4-2的相互作用较弱,与Cu(丝氨酸)(en)和Cu(PS)(2,2'-联吡啶)-几乎没有相互作用,这揭示了包括磷酸单酯基团在内的组合配体球的关键作用。结果表明,Fe2Tf或任一单价铁转铁蛋白释放铁是由于铁结合稳定性的破坏以及协同阴离子碳酸根(或草酸根)的排出。活性铜(II)配合物被假定为膜成分的模型,在细胞受体部位摄取转铁蛋白后能够从转铁蛋白中释放铁。

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