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用于黑色素瘤癌细胞靶向表面增强拉曼光谱成像和远程控制光热治疗的单链抗体修饰的金纳米笼@脂质体层纳米探针

Single-chain antibody-decorated Au nanocages@liposomal layer nanoprobes for targeted SERS imaging and remote-controlled photothermal therapy of melanoma cancer cells.

作者信息

Farahavar Ghazal, Abolmaali Samira Sadat, Nejatollahi Foroogh, Safaie Amin, Javanmardi Sanaz, Khajeh Zadeh Hossein, Yousefi Reza, Nadgaran Hamid, Mohammadi-Samani Soliman, Tamaddon Ali Mohammad, Ahadian Samad

机构信息

Pharmaceutical Nanotechnology Department, Shiraz University of Medical Sciences, Shiraz 71345, Iran.

Pharmaceutical Nanotechnology Department, Shiraz University of Medical Sciences, Shiraz 71345, Iran; Center for Nanotechnology in Drug Delivery, Shiraz University of Medical Sciences, Shiraz 71345, Iran.

出版信息

Mater Sci Eng C Mater Biol Appl. 2021 May;124:112086. doi: 10.1016/j.msec.2021.112086. Epub 2021 Mar 31.

Abstract

The development of theranostic platforms combining surface-enhanced Raman spectroscopy (SERS) imaging with NIR-stimulated photothermal therapy (PTT) is of utmost importance for the precise diagnosis and selective treatment of cancers, especially in superficial solid tumors. For this purpose, a versatile theranostic nanoprobe of liposomal layer-coated Au nanocages (AuNCs) was decorated with an anti-MUC18 single-chain antibody (scFv). 4-mercapto benzoic acid (p-MBA)-labeled AuNCs (p-AuNCs) were coated by a liposomal layer (p-AuNCs@lip), followed by conjugating anti-MUC18 scFv via post-insertion method to form immuno-liposomal layer-coated AuNCs (p-AuNCs@scFv-lip). Physicochemical characterizations of the p-AuNCs@scFv-lip were investigated by transmission electron microscopy (TEM) and UV-vis and Raman spectroscopy. Furthermore, the targeting ability and theranostic efficiency of the nanoprobe were evaluated for specific diagnosis and treatment of cancerous melanoma cells by flow cytometry, SERS mapping, and live/dead assay. The formation of lipid layer on p-AuNCs surface was confirmed by TEM imaging. After decorating the liposomal layer with scFv, a relevant red shift was observed in the UV-vis spectrum. Moreover, p-AuNCs@lip presented characteristic peaks in the Raman spectrum, which exhibited only a minor change after scFv conjugation (p-AuNCs@scFv-lip). Interestingly, the cellular uptake of AuNCs@scFv-lip by A375 cell line (MUC18) showed a 24-fold enhancement compared with SKBR3 cells (MUC18). AuNCs@scFv-lip specifically identified A375 cells from SKBR cells via SERS mapping and effectively killed A375 cells through the PTT mechanism. Taken together, this theranostic platform can provide a promising tool for both in situ diagnosis and remote-controlled thermal ablation of cancer cells.

摘要

将表面增强拉曼光谱(SERS)成像与近红外刺激光热疗法(PTT)相结合的诊疗平台的开发对于癌症的精确诊断和选择性治疗至关重要,尤其是在浅表实体瘤中。为此,一种多功能的脂质体层包被金纳米笼(AuNCs)诊疗纳米探针用抗MUC18单链抗体(scFv)进行了修饰。用脂质体层包被4-巯基苯甲酸(p-MBA)标记的AuNCs(p-AuNCs)(p-AuNCs@lip),然后通过后插入法偶联抗MUC18 scFv以形成免疫脂质体层包被的AuNCs(p-AuNCs@scFv-lip)。通过透射电子显微镜(TEM)、紫外可见光谱和拉曼光谱对p-AuNCs@scFv-lip进行了物理化学表征。此外,通过流式细胞术、SERS映射和活/死检测评估了该纳米探针针对癌性黑色素瘤细胞的靶向能力和诊疗效率。通过TEM成像证实了p-AuNCs表面脂质层的形成。在用scFv修饰脂质体层后,在紫外可见光谱中观察到相关的红移。此外,p-AuNCs@lip在拉曼光谱中呈现特征峰,在偶联scFv后(p-AuNCs@scFv-lip)仅表现出微小变化。有趣的是,A375细胞系(MUC18)对AuNCs@scFv-lip的细胞摄取与SKBR3细胞(MUC18)相比增强了24倍。AuNCs@scFv-lip通过SERS映射从SKBR细胞中特异性识别A375细胞,并通过PTT机制有效杀死A375细胞。综上所述,该诊疗平台可为癌细胞的原位诊断和远程控制热消融提供一种有前景的工具。

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