Targeting bacterial biofilm-related genes with nanoparticle-based strategies

Shima Afrasiabi, Alireza Partoazar
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Abstract

Persistent infection caused by biofilm is an urgent in medicine that should be tackled by new alternative strategies. Low efficiency of classical treatments and antibiotic resistance are the main concerns of the persistent infection due to biofilm formation which increases the risk of morbidity and mortality. The gene expression patterns in biofilm cells differed from those in planktonic cells. One of the promising approaches against biofilms is nanoparticle (NP)-based therapy in which NPs with multiple mechanisms hinder the resistance of bacterial cells in planktonic or biofilm forms. For instance, NPs such as silver (Ag), zinc oxide (ZnO), titanium dioxide (TiO2), copper oxide (Cu), and iron oxide (Fe3O4) through the different strategies interfere with gene expression of bacteria associated with biofilm. The NPs can penetrate into the biofilm structure and affect the expression of efflux pump, quorum-sensing, and adhesion-related genes, which lead to inhibit the biofilm formation or development. Therefore, understanding and targeting of the genes and molecular basis of bacterial biofilm by NPs point to therapeutic targets that make possible control of biofilm infections. In parallel, the possible impact of NPs on the environment and their cytotoxicity should be avoided through controlled exposure and safety assessments. This study focuses on the biofilm-related genes that are potential targets for the inhibition of bacterial biofilms with highly effective NPs, especially metal or metal oxide NPs.
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利用基于纳米粒子的策略靶向细菌生物膜相关基因
生物膜引起的持续感染是医学界的当务之急,应采用新的替代策略加以解决。生物膜形成导致的持续性感染增加了发病率和死亡率的风险,而传统治疗方法的低效率和抗生素耐药性是人们关注的主要问题。生物膜细胞的基因表达模式与浮游细胞不同。以纳米粒子(NP)为基础的疗法是对抗生物膜的有效方法之一,其中具有多种机制的 NPs 可阻碍浮游或生物膜形态细菌细胞的抵抗力。例如,银(Ag)、氧化锌(ZnO)、二氧化钛(TiO2)、氧化铜(Cu)和氧化铁(Fe3O4)等纳米粒子通过不同的策略干扰与生物膜相关的细菌的基因表达。NPs 可渗透到生物膜结构中,影响外排泵、法定量感应和粘附相关基因的表达,从而抑制生物膜的形成或发展。因此,了解并利用 NPs 靶向细菌生物膜的基因和分子基础,就能找到控制生物膜感染的治疗靶点。同时,应通过控制接触和安全评估来避免 NPs 对环境可能造成的影响及其细胞毒性。本研究的重点是生物膜相关基因,这些基因是利用高效 NPs(尤其是金属或金属氧化物 NPs)抑制细菌生物膜的潜在靶点。
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