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首页> 外文期刊>Journal of Medicinal Chemistry >Purification-Free Method for Preparing Technetium-99m-Labeled Multivalent Probes for Enhanced in Vivo Imaging of Saturable Systems
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Purification-Free Method for Preparing Technetium-99m-Labeled Multivalent Probes for Enhanced in Vivo Imaging of Saturable Systems

机译:制备Tech 99m标记的多价探针以增强可饱和系统体内成像的无纯化方法

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摘要

Metallic radionuclides provide target-specific radiolabeled probes for molecular imaging in radiochemical yields sufficient for administration to subjects without purification. However, unlabeled ligands in the injectate can compete for targeted molecules with radiolabeled probes, which eventually necessitates postlabeling purification. Herein we describe a "1 to 3" design to circumvent the issue by taking advantage of inherent coordination properties of technetium 99m (Tc-99m). A monovalent RGD ligand possessing an isonitrile as a coordinating moiety (CN-RGD) was reacted with [Tc-99m(CO)(3)(OH2)(3)](+) to prepare [Tc-99m(CO)(3)(CN-RGD)(3)](+) in over 95% radiochemical yields. This complex exhibited higher integrin alpha(v)beta(3) binding affinity than its unlabeled monovalent ligand, primarily due to its multivalency. This compound visualized a murine tumor without removing unlabeled ligands, while a Tc-99m-labeled monovalent probe derived from a monovalent ligand could not. The metal coordination-mediated synthesis of radiolabeled multivalent probes thereby can be a useful approach for preparing ready-to-use target-specific probes labeled with Tc-99m and other metallic radionuclides of interest.
机译:金属放射性核素为分子成像提供靶标特异性的放射性标记探针,其放射化学产率足以无需纯化即可施用于受试者。但是,注射液中未标记的配体可以与放射性标记的探针竞争靶向分子,最终需要进行标记后的纯化。在这里,我们描述了一种“ 1至3”设计,以利用99 99m(Tc-99m)的固有配位特性来规避该问题。以异腈为配位基团的一价RGD配体(CN-RGD)与[Tc-99m(CO)(3)(OH2)(3)](+)反应制备[Tc-99m(CO)(3) )(CN-RGD)(3)](+)的放射化学收率超过95%。此复合物比其未标记的单价配体表现出更高的整联蛋白α(v)beta(3)结合亲和力,主要是由于其多价。该化合物可视化了鼠类肿瘤,但未去除未标记的配体,而Tc-99m标记的源自一价配体的一价探针无法去除。因此,金属配位介导的放射性标记的多价探针的合成可以成为制备用Tc-99m和其他感兴趣的金属放射性核素标记的即用型靶标特异性探针的有用方法。

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