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Ruthenium metallopharmaceuticals

机译:钌金属药物

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The well-developed synthetic chemistry of ruthenium, particularly with ammine, amine and imine ligands, provides for many approaches to innovative new metallopharmaceuticals. Advantages of utilizing ruthenium am(m)ine complexes in drug development include, (1) reliable preparations of stable complexes with predictable structures; (2) the ability to tune ligand affinities, electron transfer and substitution rates, and reduction potentials; and (3) an increasing knowledge of the biological effects of ruthenium complexes. Many Ru(Ⅱ) and Ru(Ⅲ) amfm)ine complexes selectively bind to imine sites in biomolecules. Collectively, these lend ruthenium complexes to redox-activation and photodynamic approaches to therapy as well as the development of radio-Pharmaceuticals containing one of several radionuclides of ruthenium. Ruthenium red and the related Ru360 strongly inhibit calcium ion uptake in the mitochondria. A number of ruthenium compounds with anticancer activity appear to penetrate tumors through a transferrin-mediated process and bind to cellular DNA following intracellular activation by reduction. Ruthenium complexes exhibit both nitric oxide release and scavenging functions that can affect vasodilation and synapse firing. Simple ruthenium complexes are unusually effective in suppressing the immune response by inhibiting T cell proliferation.
机译:钌(特别是具有胺,胺和亚胺配体)的发达的合成化学方法为创新的新金属药物提供了许多方法。在药物开发中利用钌氨(m)配合物的优势包括:(1)可靠地制备具有可预测结构的稳定配合物; (2)调节配体亲和力,电子转移和取代率以及还原电位的能力; (3)对钌配合物的生物效应的认识不断增加。许多Ru(Ⅱ)和Ru(Ⅲ)amfm)配合物选择性地结合到生物分子中的亚胺位点。总的来说,这些将钌配合物用于氧化还原激活和光动力疗法,以及开发了包含钌几种放射性核素之一的放射性药物。钌红和相关的Ru360强烈抑制线粒体中钙离子的摄取。许多具有抗癌活性的钌化合物似乎通过转铁蛋白介导的过程穿透肿瘤,并在细胞内被还原激活后与细胞DNA结合。钌配合物具有一氧化氮释放和清除功能,这些功能会影响血管舒张和突触释放。简单的钌配合物通过抑制T细胞增殖在抑制免疫反应方面异常有效。

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