用于医学应用的发生器产生的68Ga的处理。

Processing of generator-produced 68Ga for medical application.

作者信息

Zhernosekov Konstantin P, Filosofov Dimitry V, Baum Richard P, Aschoff Peter, Bihl Heiner, Razbash Anatoli A, Jahn Markus, Jennewein Mark, Rösch Frank

机构信息

Institute of Nuclear Chemistry, Johannes Gutenberg-Universität Mainz, Mainz, Germany.

出版信息

J Nucl Med. 2007 Oct;48(10):1741-8. doi: 10.2967/jnumed.107.040378. Epub 2007 Sep 14.

DOI:10.2967/jnumed.107.040378

PMID:17873136

Abstract

UNLABELLED

The (68)Ge/(68)Ga generator provides an excellent source of positron-emitting (68)Ga. However, newly available "ionic" (68)Ge/(68)Ga radionuclide generators are not necessarily optimized for the synthesis of (68)Ga-labeled radiopharmaceuticals. The eluates have rather large volumes, a high concentration of H(+) (pH of 1), a breakthrough of (68)Ge, increasing with time or frequency of use, and impurities such as stable Zn(II) generated by the decay of (68)Ga, Ti(IV) as a constituent of the column material, and Fe(III) as a general impurity.

METHODS

We have developed an efficient route for the processing of generator-derived (68)Ga eluates, including the labeling and purification of biomolecules. Preconcentration and purification of the initial generator eluate are performed using a miniaturized column with organic cation-exchanger resin and hydrochloric acid/acetone eluent. The purified fraction was used for the labeling of nanomolar amounts of octreotide derivatives either in pure aqueous solution or in buffers.

RESULTS

Using the generator post-eluate processing system, >97% of the initially eluated (68)Ga activity was obtained within 4 min as a 0.4-mL volume of a hydrochloric acid/acetone fraction. The initial amount of (68)Ge(IV) was decreased by a factor of 10(4), whereas initial amounts of Zn(II), Ti(IV), and Fe(III) were reduced by factors of 10(5), 10(2), and 10, respectively. The processed (68)Ga fraction was directly transferred to solutions containing labeling precursors-for example, DOTA-dPhe(1)-Tyr(3)-octreotide (DOTATOC) (DOTA = 1,4,7,10-tetraazacyclododecane-N,N',N'',N'''-tetraacetic acid). Labeling yields of >95% were achieved within 10 min. Overall yields reached 70% at 20 min after generator elution relative to the eluted (68)Ga activity, not corrected for decay. Specific activities of (68)Ga-DOTATOC were 50 MBq/nmol using a standard protocol, reaching 450 MBq/nmol under optimized conditions.

CONCLUSION

Processing on a cation-exchanger in hydrochloric acid/acetone media represents an efficient strategy for the concentration and purification of generator-derived (68)Ga(III) eluates. The developed scheme guarantees high yields and safe preparation of injectable (68)Ga-labeled radiopharmaceuticals for routine application and is easy to automate. Thus, it is being successfully used in clinical environments and might contribute to a new direction for clinical PET, which could benefit significantly from the easy and safe availability of the radionuclide generator-derived metallic positron-emitter (68)Ga.

摘要

未标记

（68）Ge/（68）Ga发生器可提供发射正电子的（68）Ga的优质来源。然而，新上市的“离子型”（68）Ge/（68）Ga放射性核素发生器不一定针对（68）Ga标记放射性药物的合成进行了优化。洗脱液的体积相当大，H⁺浓度高（pH为1），（68）Ge有突破现象，且随着使用时间或频率增加而增多，还有诸如由（68）Ga衰变产生的稳定Zn（II）、作为柱材料成分的Ti（IV）以及作为一般杂质的Fe（III）等杂质。

方法

我们开发了一种处理发生器衍生的（68）Ga洗脱液的有效方法，包括生物分子的标记和纯化。使用装有有机阳离子交换树脂和盐酸/丙酮洗脱剂的小型柱对初始发生器洗脱液进行预浓缩和纯化。纯化后的部分用于在纯水溶液或缓冲液中标记纳摩尔量的奥曲肽衍生物。

结果

使用发生器洗脱后处理系统，在4分钟内以0.4毫升盐酸/丙酮馏分的形式获得了>97%的初始洗脱（68）Ga活度。（68）Ge（IV）的初始量降低了10⁴倍，而Zn（II）、Ti（IV）和Fe（III）的初始量分别降低了10⁵、10²和10倍。处理后的（68）Ga馏分直接转移到含有标记前体的溶液中，例如，DOTA - dPhe（1）-Tyr（3）-奥曲肽（DOTATOC）（DOTA = 1,4,7,10 - 四氮杂环十二烷 - N,N',N'',N'''-四乙酸）。在10分钟内标记产率>95%。相对于洗脱的（68）Ga活度，发生器洗脱后20分钟时的总产率达到70%，未对衰变进行校正。使用标准方案时，（68）Ga - DOTATOC的比活度为50 MBq/nmol，在优化条件下可达450 MBq/nmol。

结论

在盐酸/丙酮介质中的阳离子交换器上进行处理是一种浓缩和纯化发生器衍生的（68）Ga（III）洗脱液的有效策略。所开发的方案保证了用于常规应用的可注射（68）Ga标记放射性药物的高产率和安全制备，并且易于自动化。因此，它已在临床环境中成功应用，并可能为临床PET带来新方向，临床PET可能会从放射性核素发生器衍生的金属正电子发射体（68）Ga的简便安全可得性中显著受益。