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聚合物包被的羟基磷灰石纳米粒子的体内原位放射性标记以追踪其在小鼠体内的分布。

In Situ In Vivo radiolabeling of polymer-coated hydroxyapatite nanoparticles to track their biodistribution in mice.

机构信息

Institute of Macromolecular Chemistry AS CR, Heyrovsky Sq. 1888/2, 162 06, Prague 6, Czech Republic.

Institute of Macromolecular Chemistry AS CR, Heyrovsky Sq. 1888/2, 162 06, Prague 6, Czech Republic.

出版信息

Colloids Surf B Biointerfaces. 2019 Jul 1;179:143-152. doi: 10.1016/j.colsurfb.2019.03.057. Epub 2019 Mar 28.

DOI:10.1016/j.colsurfb.2019.03.057
PMID:30954015
Abstract

The imaging of healthy tissues and solid tumors benefits from the application of nanoparticle probes with altered pharmacokinetics, not available to low molecular weight compounds. However, the distribution and accumulation of nanoprobes in vivo typically take at least tens of hours to be efficient. For nanoprobes bearing a radioactive label, this is contradictory to the requirement of minimizing the radiation dose for patients by using as-short-as-feasible half-life radionuclides in diagnostics. Thus, we developed a two-stage diagnostic concept for monitoring long-lasting targeting effects with short-lived radioactive labels using bone-mimicking biocompatible polymer-coated and colloidally fully stabilized hydroxyapatite nanoparticles (HAP NPs) and bone-seeking radiopharmaceuticals. Within the pretargeting stage, the nonlabeled nanoparticles are allowed to circulate in the blood. Afterward, Tc-1-hydroxyethylidene-1.1-diphosphonate (Tc-HEDP) is administered intravenously for in situ labeling of the nanoparticles and subsequent single-photon emission computed tomography/computed tomography (SPECT/CT) visualization. The HAP NPs, stabilized with tailored hydrophilic polymers, are not cytotoxic in vitro, as shown by several cell lines. The polymer coating prolongs the circulation of HAP NPs in the blood. The nanoparticles were successfully labeled in vivo with Tc-HEDP, 1 and 24 h after injection, and they were visualized by SPECT/CT over time in healthy mice.

摘要

健康组织和实体瘤的成像得益于具有改变的药代动力学的纳米颗粒探针的应用,而这些探针是低分子量化合物所不具备的。然而,纳米探针在体内的分布和积累通常需要至少数十个小时才能达到高效。对于带有放射性标记的纳米探针,这与使用诊断中半衰期尽可能短的放射性核素来尽量减少患者的辐射剂量的要求相矛盾。因此,我们开发了一种两阶段诊断概念,使用类似于骨骼的生物相容性聚合物涂层和胶体完全稳定的羟磷灰石纳米颗粒(HAP NPs)和骨靶向放射性药物,使用短寿命放射性标记来监测具有长半衰期的靶向效应。在预靶向阶段,允许未标记的纳米颗粒在血液中循环。之后,静脉内给予 Tc-1-羟乙基二膦酸盐(Tc-HEDP),原位标记纳米颗粒,随后进行单光子发射计算机断层扫描/计算机断层扫描(SPECT/CT)可视化。用定制的亲水性聚合物稳定的 HAP NPs 在体外没有细胞毒性,如通过几种细胞系所示。聚合物涂层延长了 HAP NPs 在血液中的循环时间。纳米颗粒在体内用 Tc-HEDP 成功标记,在注射后 1 和 24 小时,在健康小鼠中通过 SPECT/CT 随时间进行可视化。

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