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多功能量子点偶联免疫脂质体在体外和体内的靶向肿瘤细胞内化及成像

Targeted tumor cell internalization and imaging of multifunctional quantum dot-conjugated immunoliposomes in vitro and in vivo.

作者信息

Weng Kevin C, Noble Charles O, Papahadjopoulos-Sternberg Brigitte, Chen Fanqing F, Drummond Daryl C, Kirpotin Dmitri B, Wang Donghui, Hom Yun K, Hann Byron, Park John W

机构信息

UCSF Helen Diller Family Comprehensive Cancer Center, San Francisco, California 94115, USA.

出版信息

Nano Lett. 2008 Sep;8(9):2851-7. doi: 10.1021/nl801488u. Epub 2008 Aug 20.

DOI:10.1021/nl801488u
PMID:18712930
Abstract

Targeted drug delivery systems that combine imaging and therapeutic modalities in a single macromolecular construct may offer advantages in the development and application of nanomedicines. To incorporate the unique optical properties of luminescent quantum dots (QDs) into immunoliposomes for cancer diagnosis and treatment, we describe the synthesis, biophysical characterization, tumor cell-selective internalization, and anticancer drug delivery of QD-conjugated immunoliposome-based nanoparticles (QD-ILs). Pharmacokinetic properties and in vivo imaging capability of QD-ILs were also investigated. Freeze-fracture electron microscopy was used to visualize naked QDs, liposome controls, nontargeted QD-conjugated liposomes (QD-Ls), and QD-ILs. QD-ILs prepared by insertion of anti-HER2 scFv exhibited efficient receptor-mediated endocytosis in HER2-overexpressing SK-BR-3 and MCF-7/HER2 cells but not in control MCF-7 cells as analyzed by flow cytometry and confocal microscopy. In contrast, nontargeted QD-Ls showed minimal binding and uptake in these cells. Doxorubicin-loaded QD-ILs showed efficient anticancer activity, while no cytotoxicity was observed for QD-ILs without chemotherapeutic payload. In athymic mice, QD-ILs significantly prolonged circulation of QDs, exhibiting a plasma terminal half-life ( t 1/2) of approximately 2.9 h as compared to free QDs with t 1/2 < 10 min. In MCF-7/HER2 xenograft models, localization of QD-ILs at tumor sites was confirmed by in vivo fluorescence imaging.

摘要

在单个大分子构建体中结合成像和治疗方式的靶向药物递送系统可能在纳米药物的开发和应用中具有优势。为了将发光量子点(QDs)的独特光学特性整合到免疫脂质体中用于癌症诊断和治疗,我们描述了基于量子点共轭免疫脂质体的纳米颗粒(QD-ILs)的合成、生物物理表征、肿瘤细胞选择性内化和抗癌药物递送。还研究了QD-ILs的药代动力学特性和体内成像能力。冷冻断裂电子显微镜用于观察裸量子点、脂质体对照、非靶向量子点共轭脂质体(QD-Ls)和QD-ILs。通过流式细胞术和共聚焦显微镜分析,插入抗HER2单链抗体片段(scFv)制备的QD-ILs在HER2过表达的SK-BR-3和MCF-7/HER2细胞中表现出高效的受体介导的内吞作用,但在对照MCF-7细胞中未观察到。相比之下,非靶向QD-Ls在这些细胞中的结合和摄取极少。负载阿霉素的QD-ILs显示出有效的抗癌活性,而没有化疗药物负载的QD-ILs未观察到细胞毒性。在无胸腺小鼠中,QD-ILs显著延长了量子点的循环时间,与半衰期t1/2 < 10分钟的游离量子点相比,其血浆末端半衰期(t1/2)约为2.9小时。在MCF-7/HER2异种移植模型中,通过体内荧光成像证实了QD-ILs在肿瘤部位的定位。

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