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模拟宿主防御肽的β-肽聚合物通过干扰群体感应并同时杀死单个细菌,作为一种双模式抗菌剂。

Host-Defense-Peptide-Mimicking β-Peptide Polymer Acting as a Dual-Modal Antibacterial Agent by Interfering Quorum Sensing and Killing Individual Bacteria Simultaneously.

作者信息

Li Wanlin, Xiao Ximian, Qi Yuchen, Lin Xiuhui, Hu Huiqun, Shi Minqi, Zhou Min, Jiang Weinan, Liu Longqiang, Chen Kang, Wang Kai, Liu Runhui, Zhou Min

机构信息

Department of Respiratory and Critical Care Medicine, the Fourth Affiliated Hospital, Zhejiang University School of Medicine, Yiwu 223300, China.

University-University of Edinburgh Institute (ZJU-UoE Institute), Zhejiang University School of Medicine, Zhejiang University, Haining 314400, China.

出版信息

Research (Wash D C). 2023;6:0051. doi: 10.34133/research.0051. Epub 2023 Mar 14.

Abstract

Host defense peptides (HDPs) are one of the potentially promising agents for infection diseases due to their broad spectrum and low resistance rate, but their clinical applications are limited by proteolytic instability, high-cost, and complicated synthesis process. Here, we report a host-defense-peptide-mimicking β-peptide polymer that resists proteolysis to have enhanced the activity under physiological conditions, excellent antimicrobial efficiency even at high density of bacteria, and low cost for preparation. The β-peptide polymer demonstrated quorum sensing (QS) interference and bactericidal effect against both bacterial communities and individual bacterium to simultaneously block bacterial communication and disrupt bacterial membranes. The hierarchical QS network was suppressed, and main QS signaling systems showed considerably down-regulated gene expression, resulting in excellent biofilm eradication and virulence reduction effects. The dual-modal antibacterial ability possessed excellent therapeutic effects in pneumonia, which could inhibit biofilm formation and exhibit better antibacterial and anti-inflammatory efficiency than clinically used antibiotics, levofloxacin. Furthermore, the β-peptide polymer also showed excellent therapeutic effect pyogenic liver abscess. Together, we believed that the β-peptide polymer had a feasible clinical potential to treat bacterial infection diseases.

摘要

宿主防御肽(HDPs)因其广谱性和低耐药率而成为治疗感染性疾病最具潜力的药物之一,但其临床应用受到蛋白水解不稳定性、高成本和复杂合成过程的限制。在此,我们报道了一种模拟宿主防御肽的β-肽聚合物,其具有抗蛋白水解能力,在生理条件下活性增强,即使在细菌高密度时也具有出色的抗菌效率,且制备成本低。该β-肽聚合物表现出群体感应(QS)干扰以及对细菌群落和单个细菌的杀菌作用,可同时阻断细菌通讯并破坏细菌膜。分级QS网络受到抑制,主要QS信号系统的基因表达显著下调,从而产生出色的生物膜清除和毒力降低效果。这种双模式抗菌能力在肺炎治疗中具有出色的疗效,能够抑制生物膜形成,并且比临床使用的抗生素左氧氟沙星表现出更好的抗菌和抗炎效率。此外,β-肽聚合物在化脓性肝脓肿治疗中也显示出出色的疗效。我们认为,β-肽聚合物在治疗细菌感染性疾病方面具有可行的临床潜力。

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