期刊
ACS OMEGA
卷 5, 期 44, 页码 28615-28620出版社
AMER CHEMICAL SOC
DOI: 10.1021/acsomega.0c03551
关键词
-
资金
- National Institutes of Health [R01CA112503]
We have developed structurally unique bifunctional chelators in the NETA, NE3TA, and DEPA series for potential radiopharmaceutical applications. As part of our continued research efforts to generate efficient bifunctional chelators for targeted radionuclide therapy and imaging of various diseases, we designed a scorpion-like chelator that is proposed to completely saturate the coordination spheres of Y(III) and Lu(III). We herein report the synthesis and evaluation of a new chelator (3p-C-NEPA) with 10 donor groups for complexation with beta-emitting radionuclides( )(90)Y(III), Y-86(III), and Lu-1(77)(III). The chelator was synthesized and evaluated for radiolabeling kinetics with the readily available radioisotopes Y-90 and Lu-177, and the corresponding Y-90 or Lu-177-radiolabeled complexes were evaluated for in vitro stability in human serum and in vivo complex stability in mice. The new chelator rapidly bound Y-90 or Lu-177 and formed a stable complex with the radionuclides. The new chelator 3p-C-NEPA radiolabeled with either Y-90 or Lu-177 remains stable in human serum without dissociation for 10 days. Lu-177-labeled 3p-C-NEPA produced a favorable in vivo biodistribution profile in normal mice.
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