生物正交化学
体内
化学
预定位
纳米颗粒
单核吞噬细胞系统
细胞内
纳米技术
纳米医学
体内分布
生物物理学
临床前影像学
四嗪
生物分子
氧化铁纳米粒子
亚细胞定位
细胞
磁性纳米粒子
细胞外
离体
分子成像
作者
Yun Gao,Xiaotong Wang,Can Chen,Lei Chen,Xiaoyi Cao,Mengyao Wu,Yi Zhou,Jianfeng Zeng,Mingyuan Gao
标识
DOI:10.1002/adhm.202503438
摘要
Radiolabeled nanoparticles hold great promise in precision medicine due to its versatile applications in disease imaging and therapy. However, its clinical translation is often hindered by excessive accumulation in reticuloendothelial system organs, particularly the liver, which can lead to radiation-induced toxicity. Herein, an in vivo selective radiolabeling strategy is reported that exploits the distinct subcellular fates of nanoparticles in tumors versus liver. A biorthogonal nanosystem composed of trans-cyclooctene (TCO)-functionalized iron oxide nanoparticles (Fe3O4@TCO) and a radiolabeled tetrazine probe (177Lu-DOTA-Tz) is constructed to validate this concept. Owing to the hydrophilic nature, 177Lu-DOTA-Tz cannot penetrate cell membranes, resulting in spatially restricted bioorthogonal labeling in the extracellular space. At tumor sites, Fe3O4@TCO nanoparticles accumulate via the enhanced permeability and retention effect and remain accessible for efficient binding with 177Lu-DOTA-Tz. In contrast, in the liver, nanoparticles are predominantly internalized by liver cells, and its intracellular localization prevents interaction with the probe, thereby minimizing hepatic radiation retention. By harnessing these subcellular distribution differences, the approach achieves selective in vivo radiolabeling and significantly improves the tumor-to-liver radiation ratio. This study provides a biologically informed strategy for designing radiolabeled nanoplatforms with enhanced safety profiles for theranostic applications.
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