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RGD peptide functionalized and reconstituted high-density lipoprotein nanoparticles as a versatile and multimodal tumor targeting molecular imaging probe

机译:RGD肽功能化和重构的高密度脂蛋白纳米颗粒作为一种多功能的多峰肿瘤靶向分子成像探针

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摘要

High density lipoprotein (HDL), an endogenous nanoparticle, transports fat throughout the body and is capable of transferring cholesterol from atheroma in the vessel wall to the liver. In the present study, we utilized HDL as a multimodal nanoparticle platform for tumor targeting and imaging via nonspecific accumulation and specific binding to angiogenically activated blood vessels. We reconstituted HDL (rHDL) with amphiphilic gadolinium chelates and fluorescent dyes. To target angiogenic endothelial cells, rHDL was functionalized with αvβ3-integrin-specific RGD peptides (rHDL-RGD). Nonspecific RAD peptides were conjugated to rHDL nanoparticles as a control (rHDL-RAD). It was observed in vitro that all 3 nanoparticles were phagocytosed by macrophages, while αvβ3-integrin-specific rHDL-RGD nanoparticles were preferentially taken up by endothelial cells. The uptake of nanoparticles in mouse tumors was evaluated in vivo using near infrared (NIR) and MR imaging. All nanoparticles accumulated in tumors but with very different accumulation/binding kinetics as observed by NIR imaging. Moreover, confocal microscopy revealed rHDL-RGD to be associated with tumor endothelial cells, while rHDL and rHDL-RAD nanoparticles were mainly found in the interstitial space. This study demonstrates the ability to reroute HDL from its natural targets to tumor blood vessels and its potential for multimodal imaging of tumor-associated processes.—Chen, W., Jarzyna, P. A., van Tilborg, G. A. F., Nguyen, V. A., Cormode, D. P., Klink, A., Griffioen, A. W., Randolph, G. J., Fisher, E. A., Mulder, W. J. M., Fayad, Z. A. RGD peptide functionalized and reconstituted high-density lipoprotein nanoparticles as a versatile and multimodal tumor targeting molecular imaging probe.
机译:高密度脂蛋白(HDL)是一种内源性纳米颗粒,可将脂肪转运至整个身体,并能够将胆固醇从血管壁的动脉粥样硬化转移至肝脏。在本研究中,我们利用HDL作为多峰纳米颗粒平台,通过非特异性积累和与血管生成激活血管的特异性结合,将肿瘤靶向和成像。我们用两亲性螯合物和荧光染料重建了HDL(rHDL)。为了靶向血管生成内皮细胞,rHDL被αvβ3-整联蛋白特异性RGD肽(rHDL-RGD)功能化。将非特异性RAD肽偶联到rHDL纳米颗粒上作为对照(rHDL-RAD)。在体外观察到,所有3种纳米颗粒均被巨噬细胞吞噬,而αvβ3-整合素特异性rHDL-RGD纳米颗粒优先被内皮细胞吸收。使用近红外(NIR)和MR成像在体内评估了小鼠肿瘤中纳米颗粒的摄取。通过NIR成像观察到,所有纳米颗粒都聚集在肿瘤中,但是具有非常不同的聚集/结合动力学。此外,共聚焦显微镜显示rHDL-RGD与肿瘤内皮细胞有关,而rHDL和rHDL-RAD纳米颗粒主要存在于间隙中。这项研究证明了将HDL从其天然靶点转移至肿瘤血管的能力,以及其与肿瘤相关过程的多峰成像的潜力。—Chen,W.,Jarzyna,PA,van Tilborg,GAF,Nguyen,VA,Cormode,DP ,Klink,A.,Griffioen,AW,Randolph,GJ,Fisher,EA,Mulder,WJM,Fayad,ZA RGD肽功能化并重建了高密度脂蛋白纳米颗粒,作为一种多功能的多模式肿瘤靶向分子成像探针。

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