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多胺载体铁螯合剂:电荷的作用。

Polyamine-vectored iron chelators: the role of charge.

作者信息

Bergeron Raymond J, Bharti Neelam, Wiegand Jan, McManis James S, Yao Hua, Prokai Laszlo

机构信息

Department of Medicinal Chemistry, University of Florida, Gainesville, 32610-0485, USA.

出版信息

J Med Chem. 2005 Jun 16;48(12):4120-37. doi: 10.1021/jm048974f.

Abstract

The utility of polyamines as vectors for the intracellular transport of iron chelators is further described. Consistent with earlier results with polyamine analogues, these studies underscore the importance of charge in the design of polyamine-vectored chelators. Four polyamine conjugates are synthesized, two of terephthalic acid [N(1)-(4-carboxy)benzoylspermine (7) and its methyl ester (6)] and two of (S)-2-(2,4-dihydroxyphenyl)-4,5-dihydro-4-methyl-4-thiazolecarboxylic acid [(S)-4'-(HO)-DADFT] [(S)-4,5-dihydro-2-[2-hydroxy-4-(12-amino-5,9-diazadodecyl-oxy)phenyl]-4-methyl-4-thiazolecarboxylic acid (10) and its ethyl ester (9)]. These four molecules were evaluated in murine leukemia L1210 cells for their impact on cell proliferation (48- and 96-h IC(50) values), their ability to compete with spermidine for the polyamine transport apparatus (K(i)), and their intracellular accumulation. The data revealed that when neutral molecules (cargo fragments) were fixed to the polyamine vector, the conjugates competed well with spermidine for transport and were accumulated intracellularly to millimolar levels. However, this was not the case when the cargo fragments were negatively charged. Metabolic studies of the polyamine-vectored (S)-4'-(HO)-DADFTs in rodents indicated that not only did the expected deaminopropylation step occur, but also a surprisingly high level of oxidative deamination at the terminal primary nitrogens took place. Finally, the iron-clearing efficiency of the (S)-4'-(HO)-DADFT conjugates was determined in a bile-duct-cannulated rodent model. Attaching the ligand to a polyamine vector had a profound effect on increasing the iron-clearing efficiency of this chelator relative to its parent drug.

摘要

进一步阐述了多胺作为铁螯合剂细胞内转运载体的效用。与早期多胺类似物的研究结果一致,这些研究强调了电荷在多胺载体螯合剂设计中的重要性。合成了四种多胺缀合物,两种是对苯二甲酸的缀合物 [N(1)-(4-羧基)苯甲酰亚精胺(7)及其甲酯(6)],两种是(S)-2-(2,4-二羟基苯基)-4,5-二氢-4-甲基-4-噻唑羧酸[(S)-4'-(HO)-DADFT]的缀合物[(S)-4,5-二氢-2-[2-羟基-4-(12-氨基-5,9-二氮杂十二烷氧基)苯基]-4-甲基-4-噻唑羧酸(10)及其乙酯(9)]。在小鼠白血病L1210细胞中评估了这四种分子对细胞增殖的影响(48小时和96小时的IC50值)、它们与亚精胺竞争多胺转运装置的能力(Ki)以及它们在细胞内的积累情况。数据显示,当中性分子(货物片段)固定在多胺载体上时,缀合物与亚精胺在转运方面竞争良好,并在细胞内积累至毫摩尔水平。然而,当货物片段带负电荷时情况并非如此。对啮齿动物体内多胺载体的(S)-4'-(HO)-DADFT进行的代谢研究表明,不仅发生了预期的脱氨丙基化步骤,而且在末端伯氮处还发生了令人惊讶的高水平氧化脱氨反应。最后,在胆管插管的啮齿动物模型中测定了(S)-4'-(HO)-DADFT缀合物的铁清除效率。相对于其母体药物,将配体连接到多胺载体上对提高这种螯合剂的铁清除效率有深远影响。

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