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首页> 外文期刊>Dalton transactions: An international journal of inorganic chemistry >Design and investigation of photoactivatable platinum(iv) prodrug complexes of cisplatin
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Design and investigation of photoactivatable platinum(iv) prodrug complexes of cisplatin

机译:Cisplatin的光活超铂(IV)前药复合物的设计与研究

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摘要

Platinum(iv) carboxylate scaffolds have garnered considerable research interest because they can be engineered to function as prodrugs of clinical platinum(ii) anticancer drugs. These platinum(iv) prodrug complexes are stable and tunable, and activated by reduction to release their cytotoxic platinum(ii) cargo. Here we propose new platinum(iv) prodrug complexes designed to release cisplatin via photoreduction upon UV irradiation. The central strategy is to utilise aryl carboxylate ligands on the axial positions of that platinum(iv) scaffold that confer significant UV absorption and would stabilise carboxyl radical formation, thus favouring homolytic Pt-O bond cleavage. We isolated and identified aryl carboxyl radicals via spin-trapping and showed that the photoreduced platinum species mirror cisplatin reactivity toward DNA bases, thereby validating the efficacy of this approach.
机译:铂(IV)羧酸甲酸骨架已经获得了相当大的研究兴趣,因为它们可以被设计成用作临床铂(II)抗癌药物的前药。 这些铂(IV)前药复合物是稳定和可调谐的,通过还原激活以释放其细胞毒性铂(II)货物。 在这里,我们提出了新的铂(IV)前药复合物,设计用于通过紫外线照射通过光电释放顺铂。 中枢策略是利用芳基羧酸盐配体对透铂(IV)支架的轴向位置,该支架赋予显着的UV吸收,并将稳定羧基的形成,从而偏离均解PT-O键裂解。 我们通过旋转捕获分离和鉴定芳基羧基,并且表明光学铂物种对DNA碱基的反应性反映,从而验证了这种方法的功效。

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