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壳聚糖/环糊精表面吸附的载柚皮苷纳米胶囊增强细菌群体感应淬灭和抗生物膜活性。

Chitosan/cyclodextrin surface-adsorbed naringenin-loaded nanocapsules enhance bacterial quorum quenching and anti-biofilm activities.

作者信息

Nguyen Hao Thanh, Hensel Andreas, Goycoolea Francisco M

机构信息

Faculty of Biotechnology, Vietnam National University of Agriculture, 100000 Hanoi, Vietnam; Institute for Biology and Biotechnology of Plants, Laboratory of Nanobiotechnology, University of Münster, Schlossplatz 8, D-48143 Münster, Germany.

Institute for Pharmaceutical Biology and Phytochemistry, University of Münster, Corrensstrasse 48, D-48149 Münster, Germany.

出版信息

Colloids Surf B Biointerfaces. 2022 Mar;211:112281. doi: 10.1016/j.colsurfb.2021.112281. Epub 2021 Dec 9.

Abstract

Pathogenic bacteria use quorum sensing (QS), a cell-to-cell communication process that relies on small signaling molecules, to regulate the genetic expression that leads to several essential virulence factors such as bioluminescence, biofilm formation, bacterial motility, among other. Naringenin (NAR), a bitter and colorless flavanone ubiquitous in herbs and fruits, has been shown to inhibit QS activity in P. aeruginosa by decreasing the production of pyocyanin and elastase. In this study, to evaluate the anti-QS activity of naringenin against an E. coli Top 10 biosensor, we developed a novel core-corona nanocapsule formulation comprising surface co-adsorbed β-cyclodextrin (Captisol®) and chitosan loaded with NAR. The results showed that both the nanocapsule (NC) and nanoemulsion (NE) formulations, NAR payload associated with high efficiency , namely ~ 92.88 and ~ 67.98%, respectively. These formulations remained stable for 24 h and showed a biphasic controlled release profile in bacterial M9 medium. Captisol® was effectively immobilized on the NC's surface, resulting in a surface charge inversion from positive (~ + 42 mV) to negative (~ -32 mV) ζ-potential. The biosensor assay revealed that NC outperformed NE in quenching the QS response and the incorporation of naringenin at the NC's multifunctional surface enhanced this bioactivity. Cytotoxicity assays showed that when NAR was associated in NC (188 µM) it was not cytotoxic to Caco2 cells, by contrast with its free form, thus highlighting the cytoprotective effect of the developed formulation. Biofilm formation was inhibited up to ~ 60% in NAR-loaded NC (188 μM), indicating the synergistic effect of positively charged chitosan with the bioactivity of NAR while harnessing the NC's high surface area-to-volume ratio.

摘要

病原菌利用群体感应(QS),这是一种依赖于小信号分子的细胞间通信过程,来调节导致多种重要毒力因子(如生物发光、生物膜形成、细菌运动性等)的基因表达。柚皮素(NAR)是一种存在于草药和水果中的苦味无色黄烷酮,已被证明可通过减少绿脓菌素和弹性蛋白酶的产生来抑制铜绿假单胞菌中的群体感应活性。在本研究中,为了评估柚皮素对大肠杆菌Top 10生物传感器的抗群体感应活性,我们开发了一种新型的核-壳纳米胶囊制剂,其表面共吸附有β-环糊精(Captisol®)和负载有NAR的壳聚糖。结果表明,纳米胶囊(NC)和纳米乳液(NE)制剂中,NAR的负载效率都很高,分别约为92.88%和67.98%。这些制剂在24小时内保持稳定,并在细菌M9培养基中呈现双相控释曲线。Captisol®有效地固定在NC表面,导致表面电荷从正(约+42 mV)反转到负(约-32 mV)的ζ电位。生物传感器分析表明,NC在淬灭群体感应反应方面优于NE,并且在NC的多功能表面掺入柚皮素增强了这种生物活性。细胞毒性分析表明,当NAR与NC结合(188 μM)时,与游离形式相比,它对Caco2细胞没有细胞毒性,从而突出了所开发制剂的细胞保护作用。负载NAR的NC(188 μM)中生物膜形成被抑制高达约60%,表明带正电荷的壳聚糖与NAR的生物活性具有协同作用,同时利用了NC的高表面积与体积比。

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