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Optimization of Precursor Synthesis Conditions of (2S,4S)4-[ 18 F]FPArg and Its Application in Glioma Imaging.

Yong HuangLu ZhangMeng WangChengze LiWei ZhengHualong ChenYing LiangZehui Wu
Published in: Pharmaceuticals (Basel, Switzerland) (2022)
Although the tracer (2S,4S)4-[ 18 F]FPArg is expected to provide a powerful imaging method for the diagnosis and treatment of clinical tumors, it has not been realized due to the low yield of chemical synthesis and radiolabeling. A simple synthetic method for the radiolabeled precursor of (2S,4S)4-[ 18 F]FPArg in stable yield was obtained by adjusting the sequence of the synthetic steps. Furthermore, the biodistribution experiments confirmed that (2S,4S)4-[ 18 F]FPArg could be cleared out quickly in wild type mouse. Cell uptake experiments and U87MG tumor mouse microPET-CT imaging experiments showed that the tumor had high uptake of (2S,4S)4-[ 18 F]FPArg and the clearance was slow, but (2S,4S)4-[ 18 F]FPArg was rapidly cleared in normal brain tissue. MicroPET-CT imaging of nude mice bearing orthotopic HS683-Luc showed that (2S,4S)4-[ 18 F]FPArg can penetrate blood-brain barrier and image gliomas with a high contrast. Therefore, (2S,4S)4-[ 18 F]FPArg is expected to be further applied in the diagnosis and efficacy evaluation of clinical glioma.
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