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An alternatingly amphiphilic, resistance-resistant antimicrobial oligoguanidine with dual mechanisms of action

低聚物 抗菌剂 细菌 两亲性 DNA 抗菌肽 细胞毒性 生物物理学 作用机理 体内 生物 微生物学 生物化学 抗药性 体外 多重耐药 化学 有机化学 遗传学 生物技术 共聚物 聚合物
作者
Zhiyong Chen,Cailing Zhou,Yangfan Xu,Kang Wen,Junfeng Song,Silei Bai,Chenxuan Wu,Wei Huang,Qingyun Cai,Kai Zhou,Hui Wang,Yingjie Wang,Xinxin Feng,Yugang Bai
出处
期刊:Biomaterials [Elsevier BV]
卷期号:275: 120858-120858 被引量:36
标识
DOI:10.1016/j.biomaterials.2021.120858
摘要

The increasing number of infections caused by multi-drug resistance (MDR) bacteria is an omen of a new global challenge. As one of the countermeasures under development, antimicrobial peptides (AMPs) and AMP mimics have emerged as a new family of antimicrobial agents with high potential, due to their low resistance generation rate and effectiveness against MDR bacterial strains resulted from their membrane-disrupting mechanism of action. However, most reported AMPs and AMP mimics have facially amphiphilic structures, which may lead to undesired self-aggregation and non-specific binding, as well as increased cytotoxicity toward mammalian cells, all of which put significant limits on their applications. Here, we report an oligomer with the size of short AMPs, with both hydrophobic carbon chain and cationic groups placed on its backbone, giving an alternatingly amphiphilic structure that brings better selectivity between mammalian and bacterial cell membranes. In addition, the oligomer shows affinity toward DNA, thus it can utilize bacterial DNA located in the vulnerable nucleoid as the second drug target. Benefiting from these designs, the oligomer shows higher therapeutic index and synergistic effect with other antibiotics, while its low resistance generation rate and effectiveness on multi-drug resistant bacterial strains can be maintained. We demonstrate that this alternatingly amphiphilic, DNA-binding oligomer is not only resistance-resistant, but is also able to selectively eliminate bacteria at the presence of mammalian cells. Importantly, the oligomer exhibits good in vivo activity: it cleans all bacteria on Caenorhabditis elegans without causing apparent toxicity, and significantly improves the survival rate of mice with severely infected wounds in a mice excision wound model study.
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