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[F]Ga-rhPSMA-7/-7.3的自动化合成:200多次常规生产的结果、质量控制及经验

Automated synthesis of [F]Ga-rhPSMA-7/ -7.3: results, quality control and experience from more than 200 routine productions.

作者信息

Wurzer Alexander, Di Carlo Daniel, Herz Michael, Richter Antonia, Robu Stephanie, Schirrmacher Ralf, Mascarin Alba, Weber Wolfgang, Eiber Matthias, Schwaiger Markus, Wester Hans-Juergen

机构信息

Chair of Pharmaceutical Radiochemistry, Technical University of Munich, Walther-Meißner-Str. 3, 85748, Garching, Germany.

Department of Nuclear Medicine, Klinikum rechts der Isar, Technical University of Munich, Munich, Germany.

出版信息

EJNMMI Radiopharm Chem. 2021 Jan 23;6(1):4. doi: 10.1186/s41181-021-00120-5.

Abstract

INTRODUCTION

The radiohybrid (rh) prostate-specific membrane antigen (PSMA)-targeted ligand [F]Ga-rhPSMA-7 has previously been clinically assessed and demonstrated promising results for PET-imaging of prostate cancer. The ligand is present as a mixture of four stereoisomers ([F]Ga-rhPSMA-7.1, - 7.2, - 7.3 and - 7.4) and after a preclinical isomer selection process, [F]Ga-rhPSMA-7.3 has entered formal clinical trials. Here we report on the establishment of a fully automated production process for large-scale production of [F]Ga-rhPSMA-7/ -7.3 under GMP conditions (EudraLex).

METHODS

[F]Fluoride in highly enriched [O]HO was retained on a strong anion exchange cartridge, rinsed with anhydrous acetonitrile and subsequently eluted with a solution of [K ⊂ 2.2.2]OH in anhydrous acetonitrile into a reactor containing Ga-rhPSMA ligand and oxalic acid in DMSO. F-for-F isotopic exchange at the Silicon-Fluoride Acceptor (SiFA) was performed at room temperature, followed by dilution with buffer and cartridge-based purification. Optimum process parameters were determined on the laboratory scale and thereafter implemented into an automated synthesis. Data for radiochemical yield (RCY), purity and quality control were analyzed for 243 clinical productions (160 for [F]Ga-rhPSMA-7; 83 for [F]Ga-rhPSMA-7.3).

RESULTS

The automated production of [F]Ga-rhPSMA-7 and the single isomer [F]Ga-rhPSMA-7.3 is completed in approx. 16 min with an average RCY of 49.2 ± 8.6% and an excellent reliability of 98.8%. Based on the different starting activities (range: 31-130 GBq, 89 ± 14 GBq) an average molar activity of 291 ± 62 GBq/μmol (range: 50-450 GBq/μmol) was reached for labeling of 150 nmol (231 μg) precursor. Radiochemical purity, as measured by radio-high performance liquid chromatography and radio-thin layer chromatography, was 99.9 ± 0.2% and 97.8 ± 1.0%, respectively.

CONCLUSION

This investigation demonstrates that F-for-F isotopic exchange is well suited for the fast, efficient and reliable automated routine production of F-labeled PSMA-targeted ligands. Due to its simplicity, speed and robustness the development of further SiFA-based radiopharmaceuticals is highly promising and can be of far-reaching importance for future theranostic concepts.

摘要

引言

放射性杂交(rh)前列腺特异性膜抗原(PSMA)靶向配体[F]Ga-rhPSMA-7此前已进行临床评估,并在前列腺癌的PET成像中显示出有前景的结果。该配体以四种立体异构体([F]Ga-rhPSMA-7.1、-7.2、-7.3和-7.4)的混合物形式存在,经过临床前异构体筛选过程后,[F]Ga-rhPSMA-7.3已进入正式临床试验。在此,我们报告在药品生产质量管理规范(GMP)条件(欧盟药品生产质量管理规范指南)下建立用于大规模生产[F]Ga-rhPSMA-7/-7.3的全自动生产工艺。

方法

高度富集的[O]HO中的[F]氟化物保留在强阴离子交换柱上,用无水乙腈冲洗,随后用[K⊂2.2.2]OH在无水乙腈中的溶液洗脱到含有Ga-rhPSMA配体和草酸的二甲基亚砜(DMSO)反应釜中。在室温下于硅氟受体(SiFA)处进行F-F同位素交换,然后用缓冲液稀释并通过柱纯化。在实验室规模上确定最佳工艺参数,随后将其应用于自动合成。对243次临床生产(160次生产[F]Ga-rhPSMA-7;83次生产[F]Ga-rhPSMA-7.3)的放射化学产率(RCY)、纯度和质量控制数据进行分析。

结果

[F]Ga-rhPSMA-7和单一异构体[F]Ga-rhPSMA-7.3的自动生产约在16分钟内完成,平均RCY为49.2±8.6%,可靠性极佳,为98.8%。基于不同的起始活度(范围:31 - 130 GBq,89±14 GBq),对于150 nmol(231μg)前体的标记,平均摩尔活度达到291±62 GBq/μmol(范围:50 - 450 GBq/μmol)。通过放射性高效液相色谱法和放射性薄层色谱法测量,放射化学纯度分别为99.9±0.2%和97.8±1.0%。

结论

本研究表明F-F同位素交换非常适合快速、高效且可靠地自动常规生产F标记的PSMA靶向配体。由于其简单性、速度和稳健性,进一步开发基于SiFA的放射性药物极具前景,对未来的诊疗一体化概念可能具有深远意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6ba1/7826325/b79a68fc7660/41181_2021_120_Fig1_HTML.jpg

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