使用 Nosyl 和碘代前体进行亲核放射性氟化合成[F]FAZA

Synthesis of [F]FAZA Using Nosyl and Iodo Precursors for Nucleophilic Radiofluorination.

作者信息

Sun William, Falzon Cheryl, Naimi Ebrahim, Akbari Ali, Wiebe Leonard I, Tandon Manju, Kumar Piyush

机构信息

Medimage Bionano Technology (Suzhou) Co. Ltd., Lab 408, building 15, 8 JinFeng Road, Suzhou New District, Jiangsu Province, Postcode 215163, China.

Cyclotek (Aust) Pty Ltd., 38 Clements Avenue, Bundoora, Vic. 3083, Australia.

出版信息

Curr Radiopharm. 2019;12(1):49-57. doi: 10.2174/1874471011666181019105947.

DOI:10.2174/1874471011666181019105947

PMID:30338747

Abstract

BACKGROUND

1-α-D-(5-Deoxy-5-[18F]fluoroarabinofuranosyl)-2-nitroimidazole ([18F]FAZA) is manufactured by nucleophilic radiofluorination of 1-α-D-(2',3'-di-O-acetyl-5'-O-toluenesulfonylarabinofuranosyl)- 2-nitroimidazole (DiAcTosAZA) and alkaline deprotection to afford [18F]FAZA. High yields (>60%) under optimized conditions frequently revert to low yields (<20%) in large scale, automated syntheses. Competing side reactions and concomitant complex reaction mixtures contribute to substantial loss of product during HPLC clean-up.

OBJECTIVE

To develop alternative precursors for facile routine clinical manufacture of [18F]FAZA that are compatible with current equipment and automated procedures.

METHODS

Two new precursors, 1-α-D-(2',3'-di-O-acetyl-5'-O-(4-nitrobenzene)sulfonyl-arabinofuranosyl)-2- nitroimidazole (DiAcNosAZA) and 1-α-D-(2',3'-di-O-acetyl-5'-iodo-arabinofuranosyl)-2-nitroimidazole (DiAcIAZA), were synthesized from commercially-available 1-α-D-arabinofuranosyl-2-nitroimidazole (AZA). A commercial automated synthesis unit (ASU) was used to condition F-18 for anhydrous radiofluorination, and to radiofluorinate DiAcNosAZA and DiAcIAZA using the local standardized protocol to manufacture [18F]FAZA from AcTosAZA.

RESULTS

DiAcNosAZA was synthesized via two pathways, in recovered yields of 29% and 40%, respectively. The nosylation of 1-α-D-(2',3'-di-O-acetyl-arabinofuranosyl)-2-nitroimidazole (DiAcAZA) featured a strong competing reaction that afforded 1-α-D-(2',3'-di-O-acetyl-5'-chloro-arabinofuranosyl)-2- nitroimidazole (DiAcClAZA) in 55% yield. Radiofluorination yields were better from DiAcNosAZA and DiAcIAZA than from DiAcTosAZA, and the presence of fewer side products afforded higher purity [18F]FAZA preparations. Several radioactive and non-radioactive by products of radiofluorination were assigned tentative chemical structures based on co-chromatography with authentic reference compounds.

CONCLUSION

DiAcClAZA, a major side-product in the preparation of DiAcNosAZA, and its deprotected analogue (ClAZA), are unproven hypoxic tissue radiosensitizers. DiAcNosAZA and DiAcIAZA provided good radiofluorination yields in comparison to AcTosAZA and could become preferred [18F]FAZA precursors if the cleaner reactions can be exploited to bypass HPLC purification.

摘要

背景

1-α-D-(5-脱氧-5-[¹⁸F]氟阿拉伯呋喃糖基)-2-硝基咪唑([¹⁸F]FAZA)是通过1-α-D-(2',3'-二-O-乙酰基-5'-O-甲苯磺酰阿拉伯呋喃糖基)-2-硝基咪唑(DiAcTosAZA)的亲核放射性氟化反应及碱性脱保护反应制得[¹⁸F]FAZA。在优化条件下能获得高产率(>60%)，但在大规模自动化合成中常常会降至低产率(<20%)。竞争性副反应及随之产生的复杂反应混合物导致在高效液相色谱(HPLC)纯化过程中产品大量损失。

目的

开发适用于[¹⁸F]FAZA常规临床制备的替代前体，使其与现有设备及自动化程序兼容。

方法

从市售的1-α-D-阿拉伯呋喃糖基-2-硝基咪唑(AZA)合成了两种新的前体，即1-α-D-(2',3'-二-O-乙酰基-5'-O-(4-硝基苯)磺酰基-阿拉伯呋喃糖基)-2-硝基咪唑(DiAcNosAZA)和1-α-D-(2',3'-二-O-乙酰基-5'-碘-阿拉伯呋喃糖基)-2-硝基咪唑(DiAcIAZA)。使用商用自动化合成单元(ASU)对¹⁸F进行无水放射性氟化反应条件处理，并按照当地标准化方案对DiAcNosAZA和DiAcIAZA进行放射性氟化反应，以从AcTosAZA制备[¹⁸F]FAZA。

结果

DiAcNosAZA通过两条途径合成，产率分别为29%和40%。1-α-D-(2',3'-二-O-乙酰基-阿拉伯呋喃糖基)-2-硝基咪唑(DiAcAZA)的对硝基苯磺酰化反应存在强烈的竞争性反应，以55%的产率生成了1-α-D-(2',3'-二-O-乙酰基-5'-氯-阿拉伯呋喃糖基)-2-硝基咪唑(DiAcClAZA)。DiAcNosAZA和DiAcIAZA的放射性氟化产率优于DiAcTosAZA，且副产物较少，从而得到了纯度更高的[¹⁸F]FAZA制剂。基于与真实参考化合物的共色谱分析，确定了放射性氟化反应的几种放射性和非放射性副产物的初步化学结构。