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Cationic radionuclides and ligands for targeted therapeutic radiopharmaceuticals

机译:针对靶向治疗放射性药物的阳离子放射性核素和配体

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This review considers the already used and potential alpha- and beta-emitting cationic radionuclides for targeted radionuclide therapy. Recent results of laboratory, preclinical and clinical applications of these radionuclides are discussed. As opposed to beta-emitters, which are already used in nuclear medicine, alpha-emitters involved in targeted radiopharmaceuticals were subjected to clinical trials only recently and were found to be therapeutically effective. The review summarizes recent trends in the development of ligands as components of radiopharmaceuticals addressing specific features of short-lived cationic radionuclides applied in medicine. Despite a steadily growing number of chelating ligands, 1,4,7,10-tetraazacyclododecane-1,4,7,10-tetraacetic acid (DOTA) and diethylenetriaminepentaacetic acid (DTPA) remain the most widely used agents in nuclear medicine. The drawbacks of these compounds restrict the application of radionuclides in medicine. Variations in the macrocycle size, the introduction and modification of substituents can significantly improve the chelating ability of ligands, enhance stability of radionuclide complexes with these ligands and eliminate the influence of ligands on the affinity of biological targeting vectors.
机译:该审查考虑已经使用的和潜在的α-和β发射阳离子放射核素,用于靶向放射性核素治疗。讨论了这些放射性核素的实验室,临床前和临床应用的最新结果。与已经在核医学中使用的β发射器相反,患有靶向放射性药物的α-发射者最近仅进行了临床试验,并且发现治疗有效。该综述总结了最近为配体开发的趋势,作为解热药物的组成部分,用于解决医学中的短寿命阳离子核苷酸的特定特征。尽管较稳定地越来越多的螯合配体,但是1,4,7,10-四氮杂萘二烷-1,4,7,10-四乙酸(DOTA)和二亚乙基三胺戊酸(DTPA)仍然是核医学中最广泛使用的药剂。这些化合物的缺点限制了放射性核素在医学中的应用。取代基的宏循环尺寸的变化,取代基的引入和改性可以显着提高配体的螯合能力,提高与这些配体的放射性核素复合物的稳定性,并消除配体对生物靶向载体的亲和力的影响。

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