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Tumor Targeting and Imaging in Live Animals with Functionalized Semiconductor Quantum Rods

机译:功能化半导体量子棒在活体动物中的肿瘤靶向和成像

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In this contribution, we demonstrate that highly luminescent CdSe/CdS/ZnS quantum rods (QRs) coated with PEGylated phospholipids and conjugated with cyclic RGD peptide can be successfully used for tumor targeting and imaging in live animals. The design of these targeted luminescent probes involves encapsulation of hydrophobic CdSe/CdS/ZnS QRs with PEGylated phospholipids, followed by conjugation of these PEGylated phospholipids to ligands that specifically target the tumor vasculature. In vivo optical imaging studies in nude mice bearing pancreatic cancer xenografts, both subcutaneous and orthotopic, indicate that the QR probes accumulate at tumor sites via the cyclic RGD peptides on the QR surface binding to the αvβ3 integrins overexpressed in the tumor vasculature, following systemic injection. In vivo tumor detection studies showed no adverse effects even at a dose roughly 6.5 times higher than has been reported for in vivo imaging studies using quantum dots. Cytotoxicity studies indicated the absence of any toxic effect in the cellular and tissue levels arising from functionalized QRs. These results demonstrate the vast potential of QRs as bright, photostable, and biocompatible luminescent probes for the early diagnosis of cancer.
机译:在这一贡献中,我们证明了涂覆有聚乙二醇化磷脂并与环状RGD肽偶联的高发光CdSe / CdS / ZnS量子棒(QRs)可成功用于活体动物的肿瘤靶向和成像。这些靶向发光探针的设计涉及用聚乙二醇化磷脂包裹疏水性CdSe / CdS / ZnS QRs,然后将这些聚乙二醇化磷脂缀合到特异性靶向肿瘤脉管系统的配体上。皮下和原位携带胰腺癌异种移植物的裸鼠体内光学成像研究表明,系统性注射后,QR探针通过QR表面上的环状RGD肽与结合在肿瘤脉管中过表达的αvβ3整联蛋白结合,聚集在肿瘤部位。 。体内肿瘤检测研究显示,即使其剂量比使用量子点进行的体内成像研究所报道的剂量高约6.5倍,也没有不良影响。细胞毒性研究表明,功能化QRs不会在细胞和组织水平产生任何毒性作用。这些结果表明,QRs作为明亮,光稳定和生物相容性发光探针的巨大潜力可用于癌症的早期诊断。

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