DESI-TQ-MS imaging for ex vivo brain biodistribution assessment: evaluation of LBT-999, a ligand of the dopamine transporter (DAT)

IF 4.4 Q1 CHEMISTRY, INORGANIC & NUCLEAR EJNMMI Radiopharmacy and Chemistry Pub Date : 2024-08-27 DOI:10.1186/s41181-024-00289-5
Laurent Galineau, Emmanuelle Claude, Zuhal Gulhan, Sylvie Bodard, Sophie Sérrière, Camille Dupuy, Jérémy Monteiro, Adeline Oury, Priscila Bertevello, Gabrielle Chicheri, Johnny Vercouillie, Lydie Nadal-Desbarats, Sylvie Chalon, Antoine Lefèvre, Patrick Emond
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Abstract

Background

Selection of the most promising radiotracer candidates for radiolabeling is a difficult step in the development of radiotracer pharmaceuticals, especially for the brain. Mass spectrometry (MS) is an alternative to study ex vivo the characteristics of candidates, but most MS studies are complicated by the pharmacologic doses injected and the dissection of regions to study candidate biodistribution. In this study, we tested the ability of a triple quadrupole analyzer (TQ LC–MS/MS) to quantify low concentrations of a validated precursor of a radiotracer targeting the DAT (LBT-999) in dissected regions. We also investigated its biodistribution on brain slices using MS imaging with desorption electrospray ionization (DESI) coupled to time-of-flight (TOF) vs. TQ mass analyzers.

Results

TQ LC–MS/MS enabled quantification of LBT-999 injected at sub-tracer doses in dissected striata. DESI-MS imaging (DESI-MSI) with both analyzers provided images of LBT-999 biodistribution on sagittal slices that were consistent with positron emission tomography (PET). However, the TOF analyzer only obtained biodistribution images at a high injected dose of LBT-999, while the TQ analyzer provided biodistribution images at lower injected doses of LBT-999 with a better signal-to-noise ratio. It also allowed simultaneous visualization of endogenous metabolites such as dopamine.

Conclusions

Our results show that LC-TQ MS/MS in combination with DESI-MSI can provide important information (biodistribution, specific and selective binding) that can facilitate the selection of the most promising candidates for radiolabeling and support the development of radiotracers.

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用于体内外脑生物分布评估的 DESI-TQ-MS 成像:多巴胺转运体 (DAT) 配体 LBT-999 的评估。
背景:选择最有前途的放射性示踪剂候选药物进行放射性标记是放射性示踪剂药物开发过程中的一个困难步骤,尤其是用于脑部的放射性示踪剂。质谱法(MS)是研究候选药物体内外特性的一种替代方法,但大多数质谱法研究都因注射的药理剂量和研究候选药物生物分布的区域解剖而变得复杂。在本研究中,我们测试了三重四极杆分析仪(TQ LC-MS/MS)在解剖区域量化低浓度靶向 DAT 的放射性示踪剂(LBT-999)的能力。我们还利用解吸电喷雾离子化(DESI)与飞行时间(TOF)质量分析仪(TQ mass analyzers)的质谱成像技术研究了它在脑片上的生物分布:结果:TQ LC-MS/MS能够对解剖纹状体中以亚示踪剂剂量注入的LBT-999进行定量。使用这两种分析仪进行的DESI-MS成像(DESI-MSI)提供了LBT-999在矢状切片上的生物分布图像,与正电子发射断层扫描(PET)结果一致。不过,TOF 分析仪只能获得高注射剂量 LBT-999 的生物分布图像,而 TQ 分析仪能提供较低注射剂量 LBT-999 的生物分布图像,且信噪比更好。它还能同时显示多巴胺等内源性代谢物:我们的研究结果表明,LC-TQ MS/MS 与 DESI-MSI 结合使用可提供重要信息(生物分布、特异性和选择性结合),有助于选择最有希望进行放射性标记的候选药物,并支持放射性racers 的开发。
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来源期刊
CiteScore
7.20
自引率
8.70%
发文量
30
审稿时长
5 weeks
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