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首页> 外文期刊>Nucleosides, nucleotides and nucleic acids >Design and evaluation of 5'-modified nucleoside analogs as prodrugs for an E. coli purine nucleoside phosphorylase mutant.
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Design and evaluation of 5'-modified nucleoside analogs as prodrugs for an E. coli purine nucleoside phosphorylase mutant.

机译:设计和评估5'-修饰的核苷类似物作为大肠杆菌嘌呤核苷磷酸化酶突变体的前药。

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摘要

Our studies have led to the identification of an E. coli PNP mutant (M64V) that is able to cleave numerous 5'-modified nucleoside analogs with much greater efficiency than the wild-type enzyme. The biological activity of the three best substrates of this mutant (9-[6-deoxy-alpha-L-talofuranosyl]-6-methylpurine (methyl(talo)-MeP-R), 9-[6-deoxy-alpha-L-talofuranosyl]-2-F-adenine, and 9-[alpha-L-lyxofuranosyl]-2-F-adenine) were evaluated so that we can optimally utilize these compounds. Our results indicated that the mechanism of toxicity of methyl(talo)-MeP-R to mice was due to its cleavage to MeP by a bacterial enzyme, and that the toxicity of the two F-Ade analogs was due to their cleavage to F-Ade by mammalian methylthioadenosine phosphorylase.
机译:我们的研究导致鉴定出一种大肠杆菌PNP突变体(M64V),该突变体能够以比野生型酶更高的效率裂解许多5'-修饰的核苷类似物。该突变体的三个最佳底物(9- [6-脱氧-α-L-talofuranosyl] -6-甲基嘌呤(甲基(talo)-MeP-R),9- [6-脱氧-α-L]的生物活性-talofuranosyl] -2-F-腺嘌呤和9- [α-L-lyxofuranosyl] -2-F-腺嘌呤被评估,以便我们可以最佳地利用这些化合物。我们的结果表明,甲基(talo)-MeP-R对小鼠的毒性机制是由于其被细菌酶裂解为MeP所致,而两种F-Ade类似物的毒性是由于其对F-的裂解所致。哺乳动物的甲基苯丙氨酸腺苷磷酸化酶。

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