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普通百里香精油+妥布霉素在纳米结构类脂体载体中:一种针对铜绿假单胞菌生物膜的新方法。

Thymus vulgaris essential oil + tobramycin within nanostructured archaeolipid carriers: A new approach against Pseudomonas aeruginosa biofilms.

机构信息

Nanomedicine Research and Development Centre, Science and Technology Department, National University of Quilmes, Roque Saenz Peña 352, Bernal, B1876, Buenos Aires, Argentina.

Institute of Physics, University of São Paulo (USP), São Paulo, Brazil; Brazilian Synchrotron Light Laboratory (LNLS), Brazilian Center for Research in Energy and Materials (CNPEM), Campinas, Brazil.

出版信息

Phytomedicine. 2022 Jul 20;102:154179. doi: 10.1016/j.phymed.2022.154179. Epub 2022 May 18.

Abstract

BACKGROUND

Pseudomonas aeruginosa biofilms in the respiratory tract of patients with an excessive inflammatory context are difficult to eradicate. New medicines that simultaneously target biofilms and inflammation should be developed.

HYPOTHESIS

Co-delivery of Thymus vulgaris essential oil (EOT) and tobramycin (TB) by nanostructured archaeolipids carriers (NAC) could support nebulization as well as improve EOT and TB antioxidant, anti-inflammatory and antibiofilm activity.

METHODS

NAC were prepared by loading EOT and TB in NAC having a compritol and miglyol core, covered with a shell of archaeolipids, extracted from the hyperhalophylic archaebacteria Halorubrum tebenquichense, and Tween 80. NAC were structurally characterized, including DSC thermograms, Raman spectra, TB release profile, EOT volatilization and in vitro antioxidant activity. In addition, stability upon nebulization, autoclaving and storage were assessed. The antibiofilm activity on P. aeruginosa PAO1 established biofilm of NAC and the cytotoxicity on human lung epithelial cells and macrophage were determined, as well as intracellular reactive oxygen species (ROS) production and cytokines release on LPS stimulated cells.

RESULTS

NAC showed a size of 197 ± 16 nm with PdI of 0.3 ± 0.1 and ζ Potential of -38 ± 3 mV. Structural characterization suggested that EOT was trapped in the compritol-miglyol core and TB was distributed between the surface of nanoparticles and free in solution. NAC displayed a dual release profile of TB, a delayed release of EOT and improved EOTs in vitro antioxidant activity. While NAC preserved its structural features after nebulization, autoclaving and 18 months of storage, carriers without archaeolipids gelled at room temperature and showed a significant increase of size after the same storage time. Below cytotoxic concentration, NAC decreased bacteria viability and enhanced the disruption of established PAO1 biofilms compared to free TB and EOT. Also, the strong entrapment of EOT in NAC delayed its volatilization, decreased intracellular ROS production and maintained its anti-inflammatory activity in LPS stimulated cells.

CONCLUSION

Combination of EOT + TB within NAC result in a stable and nebulizable formulation that enhanced the antioxidant and anti-biofilm activity of free ingredients, improved their ability to decrease intracellular ROS and provided anti-inflammatory activity, at non-cytotoxic concentrations on eukaryotic cells.

摘要

背景

在炎症反应过度的患者的呼吸道中,铜绿假单胞菌生物膜难以消除。应该开发同时针对生物膜和炎症的新药。

假设

纳米结构的古生菌脂类载体(NAC)同时递送百里香精油(EOT)和妥布霉素(TB),可以支持雾化,同时提高 EOT 和 TB 的抗氧化、抗炎和抗生物膜活性。

方法

通过将 EOT 和 TB 加载到由来自嗜盐古菌 Halorubrum tebenquichense 的古生菌脂类和吐温 80 覆盖的 compritol 和 miglyol 核组成的 NAC 中制备 NAC。对 NAC 进行结构表征,包括 DSC 热谱、拉曼光谱、TB 释放曲线、EOT 挥发和体外抗氧化活性。此外,还评估了雾化、高压灭菌和储存过程中的稳定性。测定了 NAC 对铜绿假单胞菌 PAO1 建立的生物膜的抗生物膜活性以及对人肺上皮细胞和巨噬细胞的细胞毒性,以及 LPS 刺激细胞中细胞内活性氧(ROS)产生和细胞因子释放。

结果

NAC 的粒径为 197±16nm,PDI 为 0.3±0.1,ζ 电位为-38±3mV。结构特征表明,EOT 被捕获在 compritol-miglyol 核中,TB 分布在纳米粒子的表面之间,并且在溶液中自由分布。NAC 显示出 TB 的双重释放曲线、EOT 的延迟释放和体外抗氧化活性的提高。虽然 NAC 在雾化、高压灭菌和 18 个月储存后保留了其结构特征,但不含古生菌脂类的载体在室温下凝胶化,并且在相同储存时间后粒径显著增加。在低于细胞毒性浓度下,NAC 降低了细菌活力,并增强了对已建立的 PAO1 生物膜的破坏作用,与游离 TB 和 EOT 相比。此外,EOT 在 NAC 中的强包封延迟了其挥发,降低了细胞内 ROS 的产生,并在 LPS 刺激的细胞中保持了其抗炎活性。

结论

EOT+TB 在 NAC 中的组合产生了一种稳定的可雾化制剂,增强了游离成分的抗氧化和抗生物膜活性,提高了它们降低细胞内 ROS 的能力,并在真核细胞上提供了抗炎活性,浓度低于细胞毒性。

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