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首页> 外文期刊>European Journal of Medicinal Chemistry: Chimie Therapeutique >Synthesis, antimicrobial activity, attenuation of aminoglycoside resistance in MRSA, and ribosomal A-site binding of pyrene-neomycin conjugates
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Synthesis, antimicrobial activity, attenuation of aminoglycoside resistance in MRSA, and ribosomal A-site binding of pyrene-neomycin conjugates

机译:合成,抗微生物活性,MRSA中的氨基糖苷抗性的衰减,以及芘 - 新霉素缀合物的核糖体a - 位点结合

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摘要

The development of new ligands that have comparable or enhanced therapeutic efficacy relative to current drugs is vital to the health of the global community in the short and long term. One strategy to accomplish this goal is to functionalize sites on current antimicrobials to enhance specificity and affinity while abating resistance mechanisms of infectious organisms. Herein, we report the synthesis of a series of pyreneneomycin B (PYR-NEO) conjugates, their binding affinity to A-site RNA targets, resistance to aminoglycoside-modifying enzymes (AMEs), and antibacterial activity against a wide variety of bacterial strains of clinical relevance. PYR-NEO conjugation significantly alters the affinities of NEO for bacterial A-site targets. The conjugation of PYR to NEO significantly increased the resistance of NEO to AME modification. PYR-NEO conjugates exhibited broad-spectrum activity towards Gram-positive bacteria, including improved activity against NEO-resistant methicillin-resistant Staphylococcus aureus (MRSA) strains. (C) 2018 Elsevier Masson SAS. All rights reserved.
机译:相对于目前药物具有可比性或增强的治疗效果的新配体的发展对于短期和长期来说是全球社会的健康至关重要。实现这一目标的一种策略是在目前抗菌药物上挥发出现的网站,以增强传染性生物的阻力机制的特异性和亲和力。在此,我们报告了一系列芘霉素B(Pyr-neo)缀合物的合成,其对A位点RNA靶标的结合亲和力,对氨基糖苷改性酶(AME)的抗性以及针对各种细菌菌株的抗菌活性临床相关性。 Pyr-Neo缀合显着改变了Neo的亲细菌A现场靶标的亲和力。 Pyr到Neo的缀合显着增加了Neo的抗性对AME改性。 Pyr-Neo缀合物表现出朝向革兰氏阳性细菌的广谱活动,包括改善对抗新甲氧西蛋白抗金黄色葡萄球菌(MRSA)菌株的活性。 (c)2018年Elsevier Masson SAS。版权所有。

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