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In vivo tumor targeting and image-guided drug delivery with antibody-conjugated, radiolabeled mesoporous silica nanoparticles

机译:抗体偶联,放射性标记的介孔二氧化硅纳米粒子的体内肿瘤靶向和图像引导药物递送

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摘要

Since the first use of biocompatible mesoporous silica (mSiO_2) nanoparticles as drug delivery vehicles, in vivo tumor targeted imaging and enhanced anticancer drug delivery has remained a major challenge. In this work, we describe the development of functionalized mSiO_2 nanoparticles for actively targeted positron emission tomography (PET) imaging and drug delivery in 4T1 murine breast tumor-bearing mice. Our structural design involves the synthesis, surface functionalization with thiol groups, PEGylation, TRC105 antibody (specific for CD105/endoglin) conjugation, and 64Cu-labeling of uniform 80 nm sized mSiO_2 nanoparticles. Systematic in vivo tumor targeting studies clearly demonstrated that ~(64)Cu-NOTA-mSiO _2-PEG-TRC105 could accumulate prominently at the 4T1 tumor site via both the enhanced permeability and retention effect and TRC105-mediated binding to tumor vasculature CD105. As a proof-of-concept, we also demonstrated successful enhanced tumor targeted delivery of doxorubicin (DOX) in 4T1 tumor-bearing mice after intravenous injection of DOX-loaded NOTA-mSiO _2-PEG-TRC105, which holds great potential for future image-guided drug delivery and targeted cancer therapy.
机译:自从首次将生物相容性介孔二氧化硅(mSiO_2)纳米颗粒用作药物传递载体以来,体内肿瘤靶向成像和增强的抗癌药物传递一直是主要挑战。在这项工作中,我们描述了功能化的mSiO_2纳米粒子的发展,该纳米粒子用于在4T1小鼠乳腺荷瘤小鼠中主动靶向的正电子发射断层扫描(PET)成像和药物递送。我们的结构设计涉及合成,巯基表面功能化,聚乙二醇化,TRC105抗体(对CD105 / endoglin特异)偶联以及对80nm大小的均匀mSiO_2纳米颗粒进行64Cu标记。系统的体内肿瘤靶向研究清楚地表明,〜(64)Cu-NOTA-mSiO _2-PEG-TRC105可以通过增强的通透性和保留作用以及TRC105介导的与肿瘤脉管CD105的结合而明显聚集在4T1肿瘤部位。作为概念验证,我们还证明了在静脉注射负载DOX的NOTA-mSiO _2-PEG-TRC105静脉注射后,在4T1荷瘤小鼠中成功增强了针对阿霉素(DOX)的肿瘤靶向递送,这具有巨大的未来潜力引导的药物输送和靶向癌症治疗。

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