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Studies toward the development of new silicon-containing building blocks for the direct ~(18)F-labeling of peptides

机译:直接肽的〜(18)F标记新含硅结构单元的开发研究

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摘要

Silicon-containing prosthetic groups have been conjugated to peptides to allow for a single-step labeling with ~(18)F radioisotope. The fairly lipophilic di-tert-butylphenylsilane building block contributes unfavorably to the pharmacokinetic profile of bombesin conjugates. In this article, theoretical and experimental studies toward the development of more hydrophilic silicon-based building blocks are presented. Density functional theory calculations were used to predict the hydrolytic stability of di-tert-butylfluorosilanes 2-23 with the aim to improve the in vivo properties of ~(18)F-labeled silicon-containing biomolecules. As a further step toward improving the pharmacokinetic profile, hydrophilic linkers were introduced between the lipophilic di-tert-butylphenylsilane building block and the bombesin congeners. Increased tumor uptake was shown with two of these peptides in xenograft-bearing mice using positron emission tomography and biodistribution studies. The introduction of a hydrophilic linker is thus a viable approach to improve the tumor uptake of ~(18)F-labeled silicon-bombesin conjugates.
机译:含硅的修复基团已与肽缀合,以实现〜(18)F放射性同位素的单步标记。亲脂性的二叔丁基苯基硅烷结构单元不利地影响了蛙皮素缀合物的药代动力学。在这篇文章中,提出了对开发更亲水的硅基砌块的理论和实验研究。密度泛函理论计算用于预测二叔丁基氟硅烷2-23的水解稳定性,目的是提高〜(18)F标记的含硅生物分子的体内性能。作为改善药代动力学特性的进一步步骤,在亲脂性二叔丁基苯基苯基硅烷结构单元与蛙皮素同类物之间引入了亲水性接头。使用正电子发射断层扫描和生物分布研究显示,在携带异种移植物的小鼠中,使用其中的两种肽增加了肿瘤的摄取。因此,亲水性接头的引入是提高〜(18)F标记的硅-薄层结合蛋白结合物对肿瘤吸收的可行方法。

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