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Bifunctional Coupling Agents for Radiolabeling of Biomolecules and Target-Specific Delivery of Metallic Radionuclides

机译:双功能偶联剂用于生物分子的放射性标记和金属放射性核素的目标特异性传递。

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摘要

Receptor-based radiopharmaceuticals are of great current interest in early molecular imaging and radiotherapy of cancers, and provide a unique tool for target-specific delivery of radionuclides to the diseased tissues. In general, a target-specific radiopharmaceutical can be divided into four parts: targeting biomolecule (BM), pharmacokinetic modifying (PKM) linker, bifunctional coupling or chelating agent (BFC), and radionuclide. The targeting biomolecule serves as a “carrier” for specific delivery of the radionuclide. PKM linkers are used to modify radiotracer excretion kinetics. BFC is needed for radiolabeling of biomolecules with a metallic radionuclide. Different radiometals have significant difference in their coordination chemistry, and require BFCs with different donor atoms and chelator frameworks. Since the radiometal chelate can have a significant impact on physical and biological properties of the target-specific radiopharmaceutical, its excretion kinetics can be altered by modifying the coordination environment with various chelators or coligand, if needed. This review will focus on the design of BFCs and their coordination chemistry with technetium, copper, gallium, indium, yttrium and lanthanide radiometals.
机译:基于受体的放射性药物在癌症的早期分子成像和放射治疗中引起了人们的极大兴趣,并且为将放射性核素靶标特异性递送至患病组织提供了独特的工具。通常,靶标特异性放射性药物可分为四个部分:靶向生物分子(BM),药代动力学修饰(PKM)接头,双功能偶联剂或螯合剂(BFC)和放射性核素。靶向生物分子充当放射性核素特异性递送的“载体”。 PKM接头用于修饰放射性示踪剂的排泄动力学。使用金属放射性核素对生物分子进行放射性标记需要BFC。不同的放射性金属在其配位化学上有显着差异,并且需要具有不同供体原子和螯合剂骨架的BFC。由于放射性金属螯合物会对靶标特异性放射性药物的物理和生物学特性产生重大影响,因此,如果需要,可以通过使用各种螯合剂或大分子配体修饰配位环境来改变其排泄动力学。这次审查将集中于BFC的设计及其与tech,铜,镓,铟,钇和镧系元素放射性金属的配位化学。

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