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通过超疏水无定形碳酸钙-阿霉素二氧化硅纳米粒并用聚焦超声增强实体瘤中阿霉素的递送。

Enhancing Doxorubicin Delivery in Solid Tumor by Superhydrophobic Amorphous Calcium Carbonate-Doxorubicin Silica Nanoparticles with Focused Ultrasound.

机构信息

Department of Biomedical Engineering and Environmental Sciences, National Tsing Hua University, No. 101, Section 2, Kuang-Fu Road, Hsinchu 30013, Taiwan.

Department of Biomedical Engineering, National Cheng Kung University, No. 1, University Road, Tainan 701, Taiwan.

出版信息

Mol Pharm. 2022 Nov 7;19(11):3894-3905. doi: 10.1021/acs.molpharmaceut.2c00384. Epub 2022 Aug 26.

DOI:10.1021/acs.molpharmaceut.2c00384
PMID:36018041
Abstract

The current approach of delivering chemotherapy pH-sensitive amorphous calcium carbonate-doxorubicin silica nanoparticles (ADS NPs) faces the challenge of insufficient drug dose due to drug instability within the bloodstream and poor tumor penetration. To overcome these long-standing obstacles, we proposed a superhydrophobic coating on the surface of the ADS NPs that could be easily modified fluorination (ADSF NPs). The surface of fluorinated ADS NPs was further modified with a phospholipid layer to reduce aggregation and improve biocompatibility (ADSFL NPs). The contact angle and mean size of ADSFL NPs were 30.2 ± 4.4° and 353.1 ± 54.2 nm, respectively. The superhydrophobic layer generated interfacial nanobubbles on the outer shell of the NPs that reduced water-induced leakage of doxorubicin (DOX) sevenfold compared with the uncoated group and induced a cavitation effect upon ultrasound (US) sonication. Moreover, release of DOX from the ADSFL NPs could be triggered by US, and this release was further improved 1.6-fold in acidic aqueous conditions, indicating that the ADSFL NPs retained pH responsiveness. Enhanced sonography contrast and histological examination demonstrated that US could trigger cavitation activities from ADSFL NPs to induce vessel disruption and enhance the fluorescence intensity of DOX within the tumor region threefold under US imaging guidance compared with the ADSFL NPs-only group.

摘要

目前,递送化疗药物的方法是 pH 敏感的无定形碳酸钙-阿霉素二氧化硅纳米粒子(ADS NPs),但由于药物在血液中的不稳定性和肿瘤穿透性差,存在药物剂量不足的问题。为了克服这些长期存在的障碍,我们在 ADS NPs 的表面提出了一种超疏水涂层,可以轻松进行氟化修饰(ADSF NPs)。氟化 ADS NPs 的表面进一步用磷脂层进行修饰,以减少聚集并提高生物相容性(ADSFL NPs)。ADSFL NPs 的接触角和平均粒径分别为 30.2±4.4°和 353.1±54.2nm。超疏水层在 NPs 的外壳上产生界面纳米气泡,使阿霉素(DOX)的水诱导泄漏减少了七倍,与未涂层组相比,并在超声(US)声处理时诱导空化效应。此外,DOX 可以从 ADSFL NPs 中被 US 触发释放,并且在酸性水条件下进一步提高了 1.6 倍,表明 ADSFL NPs 保持 pH 响应性。增强的超声造影和组织学检查表明,US 可以从 ADSFL NPs 中引发空化活动,从而在 US 成像引导下,与仅用 ADSFL NPs 组相比,在肿瘤区域内破坏血管,并将 DOX 的荧光强度提高三倍。

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