(89)Zr 标记顺磁奥曲肽脂质体用于癌症的 PET-MR 成像。

(89)Zr-labeled paramagnetic octreotide-liposomes for PET-MR imaging of cancer.

机构信息

Molecular Pharmacology and Chemistry Program, Memorial Sloan-Kettering Cancer Center, 1275 York Avenue, Box 16, New York, New York, 10065, USA.

出版信息

Pharm Res. 2013 Mar;30(3):878-88. doi: 10.1007/s11095-012-0929-8. Epub 2012 Dec 7.

DOI:10.1007/s11095-012-0929-8

PMID:23224977

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3578092/

Abstract

PURPOSE

Dual-modality PET/MR platforms add a new dimension to patient diagnosis with high resolution, functional, and anatomical imaging. The full potential of this emerging hybrid modality could be realized by using a corresponding dual-modality probe. Here, we report pegylated liposome (LP) formulations, housing a MR T(1) contrast agent (Gd) and the positron-emitting (89)Zr (half-life: 3.27 days), for simultaneous PET and MR tumor imaging capabilities.

METHODS

(89)Zr oxophilicity was unexpectedly found advantageous for direct radiolabeling of preformed paramagnetic LPs. LPs were conjugated with octreotide to selectively target neuroendocrine tumors via human somatostatin receptor subtype 2 (SSTr2). (89)Zr-Gd-LPs and octreotide-conjugated homolog were physically, chemically and biologically characterized.

RESULTS

(89)Zr-LPs showed reasonable stability over serum proteins and chelator challenges for proof-of-concept in vitro and in vivo investigations. Nuclear and paramagnetic tracking quantified superior SSTr2-recognition of octreotide-LP compared to controls.

CONCLUSIONS

This study demonstrated SSTr2-targeting specificity along with direct chelator-free (89)Zr-labeling of LPs and dual PET/MR imaging properties.

摘要

目的

正电子发射断层扫描/磁共振（PET/MR）双模态平台通过高分辨率、功能和解剖成像为患者诊断增添了新维度。通过使用相应的双模态探针，可以充分发挥这种新兴混合模态的潜力。在此，我们报告了载有磁共振 T(1)造影剂（Gd）和正电子发射（89）Zr（半衰期：3.27 天）的聚乙二醇化脂质体（LP）制剂，用于同时进行 PET 和 MR 肿瘤成像。

方法

出乎意料的是，（89）Zr 的亲氧性有利于直接标记预先形成的顺磁 LP。LP 与奥曲肽偶联，通过人类生长抑素受体亚型 2（SSTr2）选择性靶向神经内分泌肿瘤。（89）Zr-Gd-LP 和奥曲肽偶联的同系物在体外和体内进行了物理、化学和生物学特性研究。

结果

（89）Zr-LP 在血清蛋白和螯合剂挑战方面表现出合理的稳定性，为体外和体内研究提供了概念验证。核素和顺磁追踪定量显示，与对照相比，奥曲肽-LP 对 SSTr2 的识别具有更高的特异性。

结论

本研究证明了 SSTr2 靶向特异性，以及 LP 的直接无螯合剂（89）Zr 标记和双重 PET/MR 成像特性。

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