用于肺癌治疗的纳米颗粒的器官特异性血管递送
Organ-restricted vascular delivery of nanoparticles for lung cancer therapy.
作者信息
Bölükbas Deniz A, Datz Stefan, Meyer-Schwickerath Charlotte, Morrone Carmela, Doryab Ali, Gößl Dorothee, Vreka Malamati, Yang Lin, Argyo Christian, van Rijt Sabine H, Lindner Michael, Eickelberg Oliver, Stoeger Tobias, Schmid Otmar, Lindstedt Sandra, Stathopoulos Georgios T, Bein Thomas, Wagner Darcy E, Meiners Silke
机构信息
Comprehensive Pneumology Center (CPC), University Hospital Ludwig-Maximilians University, and Helmholtz Zentrum München, Munich, Germany. Member of the German Center for Lung Research (DZL), 81377 Munich, Germany; Lung Bioengineering and Regeneration, Dept of Experimental Medical Sciences, Stem Cell Centre, Wallenberg Center for Molecular Medicine, Lund University Cancer Centre (LUCC), Lund University, 22362 Lund, Sweden.
Department of Chemistry and Center for NanoScience (CeNS), University of Munich (LMU) 81377 Munich, Germany.
出版信息
Adv Ther (Weinh). 2020 May 13;3(7). doi: 10.1002/adtp.202000017. eCollection 2020 Jul.
Nanoparticle-based targeted drug delivery holds promise for treatment of cancers. However, most approaches fail to be translated into clinical success due to ineffective tumor targeting in vivo. Here, the delivery potential of mesoporous silica nanoparticles (MSN) functionalized with targeting ligands for EGFR and CCR2 is explored in lung tumors. The addition of active targeting ligands on MSNs enhances their uptake in vitro but fails to promote specific delivery to tumors in vivo, when administered systemically via the blood or locally to the lung into immunocompetent murine lung cancer models. Ineffective tumor targeting is due to efficient clearance of the MSNs by the phagocytic cells of the liver, spleen, and lung. These limitations, however, are successfully overcome using a novel organ-restricted vascular delivery (ORVD) approach. ORVD in isolated and perfused mouse lungs of Kras-mutant mice enables effective nanoparticle extravasation from the tumor vasculature into the core of solid lung tumors. In this study, ORVD promotes tumor cell-specific uptake of nanoparticles at cellular resolution independent of their functionalization with targeting ligands. Organ-restricted vascular delivery thus opens new avenues for optimized nanoparticles for lung cancer therapy and may have broad applications for other vascularized tumor types.
基于纳米颗粒的靶向药物递送在癌症治疗方面具有前景。然而,由于体内肿瘤靶向无效,大多数方法未能转化为临床成功。在此,研究了用针对表皮生长因子受体(EGFR)和趋化因子受体2(CCR2)的靶向配体功能化的介孔二氧化硅纳米颗粒(MSN)在肺肿瘤中的递送潜力。在MSN上添加活性靶向配体可增强其体外摄取,但当通过血液全身给药或局部给予免疫活性小鼠肺癌模型的肺部时,未能促进其在体内向肿瘤的特异性递送。肿瘤靶向无效是由于肝脏、脾脏和肺的吞噬细胞对MSN的有效清除。然而,使用一种新型的器官限制性血管递送(ORVD)方法成功克服了这些限制。在Kras突变小鼠的离体灌注肺中,ORVD可使纳米颗粒有效地从肿瘤脉管系统外渗到实体肺肿瘤核心。在本研究中,ORVD以细胞分辨率促进纳米颗粒对肿瘤细胞的特异性摄取,而与它们用靶向配体的功能化无关。因此,器官限制性血管递送为优化用于肺癌治疗的纳米颗粒开辟了新途径,并且可能对其他血管化肿瘤类型具有广泛应用。
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