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Recent developments on 3-hydroxy-4-pyridinones with respect to their clinical applications Mono and combined ligand approaches

机译:3-羟基-4-吡啶酮在临床应用方面的最新进展

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There has been considerable research effort invested in the discovery and development of chelators for the treatment of serious pathological disorders associated with iron (or aluminium) overload in the past two decades. A series of 3-hydroxy-4-pyridinone (3,4-HP) iron-ligands, in particular bis-(3,4-HP)s and mono-(3,4-HP)s were developed by exploring their polydenticity and/or bifunctionality. These compounds were assessed for their physicochemical and biological properties such as the chelating ability for M~(3+) hard metal ions (M = Fe, Al, Ga), the lipophilicity (log P) and the metal-clearing efficiency (MCE) from most organs in mice pre-loaded with ~(67)Ga, as a model of Fe-overload. Although the solution chemistry and the in vivo studies have been performed with individual ligands, a ligand combination strategy with the bis- and mono-(3,4-HP) was adopted to improve the scavenger power based on differences on their cellular-compartment accessibility. The results lead to key recommendations useful in chelator design strategies because there are significant differences in chelating affinity and MCE in mice between the bis-HP and the mono-HP ligands. The extra-functional groups of the compounds have a profound effect on log P, MCE and organ distribution, and so they can be targeted to organs compromised in iron-overload disease, for example, the liver or the brain. The coadjuvation or synergistic effects of the ligand combination is supported by the observed improvements on metal excretion in bioassays.
机译:在过去的二十年中,已经投入了大量的研究努力来发现和开发用于治疗与铁(或铝)超负荷有关的严重病理疾病的螯合剂。通过探索多羟基的性质,开发了一系列3-羟基-4-吡啶酮(3,4-HP)铁配体,特别是双-(3,4-HP)和单-(3,4-HP)和/或双功能。对这些化合物的理化和生物学特性进行了评估,例如对M〜(3+)硬金属离子的螯合能力(M = Fe,Al,Ga),亲脂性(log P)和金属清除效率(MCE)预先加载〜(67)Ga的小鼠大多数器官中的蛋白质,作为Fe超载的模型。尽管已对单个配体进行了溶液化学和体内研究,但是基于双-和单-(3,4-HP)的配体组合策略仍可根据其细胞室可及性的差异来提高清除剂的能力。 。结果导致了对螯合剂设计策略有用的关键建议,因为在双-HP和单-HP配体之间,小鼠的螯合亲和力和MCE有显着差异。该化合物的超功能基团对log P,MCE和器官分布具有深远的影响,因此它们可以靶向铁超载疾病中受损的器官,例如肝脏或大脑。在生物测定中观察到的对金属排泄的改善支持了配体组合的共轭化或协同作用。

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