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具有金属圆顶层的模块化载药纳米胶囊作为获得协同治疗生物学活性的平台。

Modular Drug-Loaded Nanocapsules with Metal Dome Layers as a Platform for Obtaining Synergistic Therapeutic Biological Activities.

机构信息

Institute for Drug Research (IDR), School of Pharmacy, Faculty of Medicine, The Hebrew University of Jerusalem, 9112102 Jerusalem, Israel.

Catalan Institute of Nanoscience and Nanotechnology (ICN2), CSIC and BIST, Campus UAB, 08193 Bellaterra, Barcelona, Spain.

出版信息

ACS Appl Mater Interfaces. 2023 Nov 1;15(43):50330-50343. doi: 10.1021/acsami.3c07188. Epub 2023 Oct 20.

Abstract

Multifunctional drug-loaded polymer-metal nanocapsules have attracted increasing attention in drug delivery due to their multifunctional potential endowed by drug activity and response to physicochemical stimuli. Current chemical synthesis methods of polymer/metal capsules require specific optimization of the different components to produce particles with precise properties, being particularly complex for Janus structures combining polymers and ferromagnetic and highly reactive metals. With the aim to generate tunable synergistic nanotherapeutic actuation with enhanced drug effects, here we demonstrate a versatile hybrid chemical/physical fabrication strategy to incorporate different functional metals with tailored magnetic, optical, or chemical properties on solid drug-loaded polymer nanoparticles. As archetypical examples, we present poly(lactic--glycolic acid) (PLGA) nanoparticles (diameters 100-150 nm) loaded with paclitaxel, indocyanine green, or erythromycin that are half-capped by either Fe, Au, or Cu layers, respectively, with application in three biomedical models. The Fe coating on paclitaxel-loaded nanocapsules permitted efficient magnetic enhancement of the cancer spheroid assembly, with 40% reduction of the cross-section area after 24 h, as well as a higher paclitaxel effect. In addition, the Fe-PLGA nanocapsules enabled external contactless manipulation of multicellular cancer spheroids with a speed of 150 μm/s. The Au-coated and indocyanine green-loaded nanocapsules demonstrated theranostic potential and enhanced anticancer activity in vitro and in vivo due to noninvasive fluorescence imaging with long penetration near-infrared (NIR) light and simultaneous photothermal-photodynamic actuation, showing a 3.5-fold reduction in the tumor volume growth with only 5 min of NIR illumination. Finally, the Cu-coated erythromycin-loaded nanocapsules exhibited enhanced antibacterial activity with a 2.5-fold reduction in the MIC50 concentration with respect to the free or encapsulated drug. Altogether, this technology can extend a nearly unlimited combination of metals, polymers, and drugs, thus enabling the integration of magnetic, optical, and electrochemical properties in drug-loaded nanoparticles to externally control and improve a wide range of biomedical applications.

摘要

多功能载药聚合物-金属纳米胶囊由于其药物活性和对外界物理化学刺激的响应赋予的多功能潜力,在药物传递领域引起了越来越多的关注。目前聚合物/金属胶囊的化学合成方法需要对不同的成分进行特定的优化,以产生具有精确性能的颗粒,对于结合聚合物和铁磁体以及高反应性金属的 Janus 结构尤其复杂。为了产生具有增强药物效果的可调谐协同纳米治疗触发作用,我们在这里展示了一种通用的混合化学/物理制造策略,将具有定制磁性、光学或化学性质的不同功能金属纳入载药聚合物纳米颗粒中。作为典型例子,我们提出了负载紫杉醇、吲哚菁绿或红霉素的聚(乳酸-乙醇酸)(PLGA)纳米颗粒(直径 100-150nm),分别通过 Fe、Au 或 Cu 层半覆盖,分别在三个生物医学模型中应用。紫杉醇载药纳米胶囊表面的 Fe 涂层可有效增强癌症球体组装的磁性,24 小时后,横截面积减少了 40%,紫杉醇效果也更高。此外,Fe-PLGA 纳米胶囊能够以 150μm/s 的速度对外接触式操控多细胞癌症球体。Au 涂层和负载吲哚菁绿的纳米胶囊由于具有非侵入性荧光成像功能,可实现长近红外(NIR)光穿透,同时进行光热-光动力触发,表现出体外和体内增强的抗癌活性和治疗潜力,NIR 光照 5 分钟即可使肿瘤体积缩小 3.5 倍。最后,Cu 涂层的载红霉素纳米胶囊表现出增强的抗菌活性,MIC50 浓度相对于游离或包封药物降低了 2.5 倍。总之,该技术可以扩展几乎无限的金属、聚合物和药物组合,从而可以在载药纳米颗粒中集成磁性、光学和电化学特性,以对外控制和改善广泛的生物医学应用。

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