首页> 外文期刊>Nuclear Medicine Communications >Radiolabelling morpholinos with 188Re tricarbonyl provides improved in vitro and in vivo stability to re-oxidation.
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Radiolabelling morpholinos with 188Re tricarbonyl provides improved in vitro and in vivo stability to re-oxidation.

机译:用188Re三羰基放射性标记吗啉代可提高体外和体内再氧化的稳定性。

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BACKGROUND: For pretargeting and other nuclear medicine applications, it may eventually be useful to radiolabel phosphodiamidate morpholinos (MORFs) with therapeutic radionuclides such as 188Re. However, by preparing 188Re-MORFs labelled conventionally with MAG3 as chelator, we have observed unacceptable levels of oxidation to perrhenate in vitro and in vivo in mice. OBJECTIVE: To improve upon stability, tricarbonyl labelling was considered since tricarbonyl complexes are thought to stabilize metals in low oxidation states. METHODS: An amine derivatized 25 mer MORF was conjugated with either NHS-MAG3 or NHS-Hynic. The MAG3 conjugated MORF was radiolabelled conventionally with 188Re while the Hynic conjugated MORF was radiolabelled through its tricarbonyl intermediate. Using a commercial kit modified with additional reducing agent over that required for the preparation of the 99mTc tricarbonyl complex [99mTc(CO)3(H2O)3]+, we demonstrated that the equivalent 188Re tricarbonyl, [188Re(CO)3(H2O)3]+, could be prepared. Simple incubation at elevated temperatures with the Hynic conjugated MORF then provided 188Re-(CO)3-Hynic-MORF. Confirmation was achieved by a shift assay using a complementary MORF conjugated polymer and size exclusion HPLC. To evaluate the relative stability of the tricarbonyl labelled MORF compared to the MAG3 labelled MORF in vitro, the radiolabelled MORFs were incubated in phosphate buffer and the presence of perrhenate measured periodically by strip chromatography. Stability in vivo was evaluated by biodistribution studies in normal mice. RESULTS: The overall yields for tricarbonyl intermediates averaged greater than 90% for 99mTc and 60-80% for 188Re. Yields following subsequent labelling to Hynic-MORF were about 60-80% for 99mTc and 15-20% for 188Re. The in vitro stability results in phosphate buffer showed that 188Re-MAG3-MORF was fully oxidized by 48 h while 188Re-(CO)3-Hynic-MORF was less than 20% oxidized at that time. Similarly, the 188Re-(CO)3-Hynic-MORF biodistribution in normal mice showed lower radioactivity level in stomach, intestines and thyroid compared with 188Re-MAG3-MORF. CONCLUSION: 188Re-tricarbonyl labelling of Hynic conjugated MORFs may be considerably more stable to oxidation than the MAG3 labelled MORFs and therefore more suitable for radiotherapy trials.
机译:背景:对于预靶向和其他核医学应用,用治疗性放射性核素(如188Re)放射性标记磷酸二mid酯吗啉代(MORF)可能最终有用。但是,通过制备常规用MAG3作螯合剂标记的188Re-MORFs,我们观察到了在小鼠体内外体内氧化到高hen酸的不可接受的水平。目的:为了提高稳定性,考虑了三羰基标记,因为三羰基络合物被认为可以稳定低氧化态的金属。方法:将胺衍生的25mer MORF与NHS-MAG3或NHS-Hynic共轭。 MAG3共轭MORF通常用188Re进行放射性标记,而Hynic共轭MORF通过其三羰基中间体进行放射性标记。使用商品化试剂盒,该试剂盒用额外的还原剂改性,制备了99mTc三羰基络合物[99mTc(CO)3(H2O)3] +所需的试剂,我们证明了188Re三羰基,[188Re(CO)3(H2O) 3] +,可以准备。然后在高温下与结合Hynic的MORF进行简单孵育,即可得到188Re-(CO)3-Hynic-MORF。通过使用互补的MORF共轭聚合物的位移分析和尺寸排阻HPLC进行确认。为了评估三羰基标记的MORF在体外与MAG3标记的MORF的相对稳定性,将放射性标记的MORF在磷酸盐缓冲液中孵育,并通过带式色谱定期测量高per酸盐的存在。通过生物分布研究在正常小鼠中评估体内稳定性。结果:三羰基中间体的总收率在99mTc时平均高于90%,在188Re时高于60-80%。随后标记为Hynic-MORF的产率对于99mTc约为60-80%,对于188Re约为15-20%。在磷酸盐缓冲液中的体外稳定性结果表明,188Re-MAG3-MORF在48 h时被完全氧化,而188Re-(CO)3-Hynic-MORF在那时被氧化不到20%。同样,与188Re-MAG3-MORF相比,正常小鼠中188Re-(CO)3-Hynic-MORF的生物分布在胃,肠和甲状腺的放射性水平较低。结论:Hynic偶联的MORF的188Re-三羰基标记可能比MAG3标记的MORF的氧化稳定得多,因此更适合放疗试验。

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