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Modification at the 2′-Position of the 45-Seriesof 2-Deoxystreptamine Aminoglycoside Antibiotics To Resist Aminoglycoside ModifyingEnzymes and Increase Ribosomal Target Selectivity

机译:45系列2位置的修饰2-脱氧链胺胺氨基糖苷类抗生素对氨基糖苷类修饰的抵抗酶和增加核糖体靶标选择性

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摘要

A series of derivatives of the 4,5-disubstituted class of 2-deoxystreptamine aminoglycoside antibiotics neomycin, paromomycin, and ribostamycin was prepared and assayed for (i) their ability to inhibit protein synthesis by bacterial ribosomes and by engineered bacterial ribosomes carrying eukaryotic decoding A sites, (ii) antibacterial activity against wild type Gram negative and positive pathogens, and (iii) overcoming resistance due to the presence of aminoacyl transferases acting at the 2′-position. The presence of five suitably positioned residual basic amino groups was found to be necessary for activity to be retained upon removal or alkylation of the 2′-position amine. As alkylation of the 2′-amino group overcomes the action of resistance determinants acting at that position and in addition results in increased selectivity for the prokaryotic over eukaryotic ribosomes, it constitutes an attractive modification for introduction into next generation aminoglycosides. In the neomycin series, the installation of small (formamide) or basic (glycinamide) amido groupson the 2′-amino group is tolerated.
机译:制备了一系列4,4-二取代类的2-脱氧链胺胺糖苷抗生素新霉素,巴龙霉素和核糖霉素的衍生物,并进行了以下方面的测定:(i)它们抑制细菌核糖体和携带真核解码蛋白A的工程化细菌核糖体抑制蛋白质合成的能力。 (ii)对野生型革兰氏阴性和阳性病原体的抗菌活性,以及​​(iii)由于存在于2'位置的氨酰基转移酶而克服了耐药性。发现5个适当定位的残留碱性氨基的存在对于在2'-位胺的去除或烷基化时保持活性是必要的。由于2'-氨基的烷基化克服了在该位置上起作用的抗性决定簇的作用,并且另外导致了对原核生物比对真核生物核糖体的选择性增加,它构成了引入下一代氨基糖苷的有吸引力的修饰。在新霉素系列中,小(甲酰胺)或碱性(甘氨酰胺)酰胺基的安装2'-氨基上的α是可容忍的。

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