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首页> 外文期刊>Bioconjugate Chemistry >In Vivo Tumor-Targeted Fluorescence Imaging Using Near-Infrared Non-Cadmium Quantum Dots
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In Vivo Tumor-Targeted Fluorescence Imaging Using Near-Infrared Non-Cadmium Quantum Dots

机译:使用近红外非镉量子点的体内肿瘤靶向荧光成像

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摘要

This article reported the high tumor targeting efficacy of RGD peptide labeled near-infrared (NIR) non-cadmium quantum dots (QDs). After using poly(ethylene glycol) to encapsulate InAs/InP/ZnSe QDs (emission maximum at about 800 nm), QD800-PEG dispersed well in PBS buffer with the hydrodynamic diameter (HD) of 15.9 nm and the circulation half-life of ~29 min. After coupling QD800-PEG with arginine—glycine-aspartic acid (RGD) or arginine—alanine—aspartic acid (RAD) peptides, we used nude mice bearing subcutaneous U87MG tumor as models to test tumor-targeted fluorescence imaging. The results indicated that the tumor uptake of QD800-RGD is much higher than those of QD800-PEG and QD800-RAD. The semiquantitative analysis of the region of interest (ROI) showed a high tumor uptake of 10.7 ± 1.5%ID/g in mice injected with QD800-RGD, while the tumor uptakes of QD800-PEG and QD800-RAD were 2.9 ± 0.3%ID/g and 4.0 ± 0.5%ID/g, respectively, indicating the specific tumor targeting of QD800-RGD. The high reproducibility of bioconjunction between QDs and the RGD peptide and the feasibility of QD-RGD bioconjugates as tumor-targeted fluorescence probes warrant the successful application of QDs for in vivo molecular imaging.
机译:本文报道了RGD肽标记的近红外(NIR)非镉量子点(QD)的高肿瘤靶向功效。用聚乙二醇封装InAs / InP / ZnSe量子点(最大发射波长约800 nm)后,QD800-PEG很好地分散在PBS缓冲液中,流体动力学直径(HD)为15.9 nm,循环半衰期为〜 29分钟将QD800-PEG与精氨酸-甘氨酸-天冬氨酸(RGD)或精氨酸-丙氨酸-天冬氨酸(RAD)肽偶联后,我们使用带有皮下U87MG肿瘤的裸鼠作为模型来测试靶向肿瘤的荧光成像。结果表明,QD800-RGD的肿瘤摄取率远高于QD800-PEG和QD800-RAD。对感兴趣区域(ROI)的半定量分析显示,在注射QD800-RGD的小鼠中,肿瘤的高摄取率为10.7±1.5%ID / g,而QD800-PEG和QD800-RAD的肿瘤摄取为2.9±0.3%ID / g和4.0±0.5%ID / g,分别表示QD800-RGD的特异性肿瘤靶向。 QD和RGD肽之间生物结合的高可重复性以及QD-RGD生物结合物作为肿瘤靶向荧光探针的可行性保证了QD在体内分子成像中的成功应用。

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