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利用大分子设计优化烷基化阳离子低聚物的抗菌活性。

Exploiting Macromolecular Design To Optimize the Antibacterial Activity of Alkylated Cationic Oligomers.

机构信息

ARC Centre of Excellence in Convergent Bio-Nano Science and Technology , Monash University , 381 Royal Pde , Parkville , VIC 3052 , Australia.

Drug Delivery, Disposition and Dynamics Theme, Monash Institute of Pharmaceutical Sciences , Monash University , 381 Royal Pde , Parkville , VIC 3052 , Australia.

出版信息

Biomacromolecules. 2018 Dec 10;19(12):4629-4640. doi: 10.1021/acs.biomac.8b01317. Epub 2018 Nov 6.

Abstract

There is growing interest in synthetic polymers which co-opt the structural features of naturally occurring antimicrobial peptides. However, our understanding of how macromolecular architecture affects antibacterial activity remains limited. To address this, we investigated whether varying architectures of a series of block and statistical co-oligomers influenced antibacterial and hemolytic activity. Cu(0)-mediated polymerization was used to synthesize oligomers constituting 2-(Boc-amino)ethyl acrylate units and either diethylene glycol ethyl ether acrylate (DEGEEA) or poly(ethylene glycol) methyl ether acrylate units with varying macromolecular architecture; subsequent deprotection produced primary amine functional oligomers. Further guanylation provided an additional series of antimicrobial candidates. Both chemical composition and macromolecular architecture were shown to affect antimicrobial activity. A broad spectrum antibacterial oligomer (containing guanidine moieties and DEGEEA units) was identified that possessed promising activity (MIC = 2 μg mL) toward both Gram-negative and Gram-positive bacteria. Bacterial membrane permeabilization was identified as an important contributor to the mechanism of action.

摘要

人们对天然抗菌肽的结构特征进行模拟的合成聚合物越来越感兴趣。然而,我们对大分子结构如何影响抗菌活性的理解仍然有限。为了解决这个问题,我们研究了一系列嵌段和统计共聚物的不同结构是否会影响抗菌和溶血活性。我们使用 Cu(0)介导的聚合来合成由 2-(Boc-氨基)乙基丙烯酰胺单元和二甘醇乙醚丙烯酸酯(DEGEEA)或聚乙二醇甲基醚丙烯酸酯单元组成的低聚物,这些低聚物具有不同的大分子结构;随后的脱保护作用产生了具有伯胺官能团的低聚物。进一步的鸟嘌呤化提供了一系列额外的抗菌候选物。化学组成和大分子结构都被证明会影响抗菌活性。我们确定了一种具有广谱抗菌活性的低聚物(含有胍基和 DEGEEA 单元),对革兰氏阴性和革兰氏阳性菌均具有有前景的活性(MIC = 2 μg mL)。细菌膜通透性被认为是作用机制的一个重要贡献者。

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