首页> 外文期刊>Journal of the Chemical Society, Perkin Transactions 1 >Leaving group effects in reductively triggered fragmentation of 4-nitrobenzyl carbamates
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Leaving group effects in reductively triggered fragmentation of 4-nitrobenzyl carbamates

机译:离开基团影响还原触发引发的4-硝基苄基氨基甲酸酯碎裂

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摘要

The rates and extent of release of a series of substituted anilines from 4-nitrobenzyl carbamates, following nitro group reduction by radiolytic, enzymic and chemical methods, are reported. The yield of released anilines decreased over the pH range 4-7, but was independent of the basicity of the leaving aniline. Detailed studies of the fragmentation of one example identified the 4-hydroxylamine as the key intermediate. At pH greater than 5 the released aniline 3b condenses with a reactive 4-iminoquinomethane intermediate 4a to give amine 26, thus depleting the measurable amount of aniline 3b released. At pH less than 5 the release of amine proceeds to completion. The efficiency of reductively triggered release of anilines 7 varied with small changes in the leaving group, but this was not uniformly related to aniline basicity. The competing reaction of the released aniline 3b to form amine 26 lowers the efficiency of release of 3b. This reaction occurs at the relatively high concentrations (50 mu M) used in the study and indicates the released effector amine should be toxic at concentrations considerably lower than 50 mu M. This highlights the need for prodrugs of very potent cytotoxic effectors to be used in tumour-directed nitroreductase enzyme-prodrug therapy. [References: 23]
机译:据报道,通过放射,酶和化学方法还原硝基后,从4-硝基苄基氨基甲酸酯中释放出一系列取代苯胺的速率和程度。在4-7的pH范围内,释放的苯胺的收率下降,但与离去苯胺的碱度无关。对一个实例的断裂的详细研究确定了4-羟胺为关键中间体。在pH大于5时,释放的苯胺3b与反应性4-亚氨基喹啉甲烷中间体4a缩合,得到胺26,因此消耗了可测量量的释放的苯胺3b。在pH值小于5时,胺的释放继续进行。还原触发的苯胺释放7的效率随离去基团的微小变化而变化,但这与苯胺的碱度并不一致。释放的苯胺3b形成胺26的竞争反应降低了3b的释放效率。该反应在研究中使用的相对较高的浓度(50μM)下发生,表明所释放的效应胺在浓度明显低于50μM的情况下应该具有毒性。这突出表明需要使用非常有效的细胞毒性效应子的前药。肿瘤导向的硝基还原酶酶前药治疗。 [参考:23]

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