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Furin-Guided Intracellular 68Ga Nanoparticle Formation Enhances Tumor MicroPET Imaging.

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Positron-emission tomography (PET) is routinely used in clinic for tumor imaging with ultra high sensitivity but tumor-targeted PET imaging probes are quite few. In this work, we rationally designed a… Click to show full abstract

Positron-emission tomography (PET) is routinely used in clinic for tumor imaging with ultra high sensitivity but tumor-targeted PET imaging probes are quite few. In this work, we rationally designed a furin-responsive radiotracer Acetyl-Arg-Val-Arg-Arg-Cys(StBu)-Lys(DOTA-68Ga)-CBT (CBT-68Ga) and demonstrated that co-injection of the radiotracer with its cold analog CBT-Ga instructed the formation of 68Ga nanoparticles in furin-overexpressing MDA-MB-468 cancer cells, which significantly enhanced microPET imaging of the tumor in vivo. In vitro results showed that CBT-Ga subjected to furin-initiated CBT-Cys condensation reaction and self-assembly to form the nanoparticles CBT-Ga-NPs with an average diameter of 258.3 nm. In vivo microPET imaging results indicate that the mice co-injected with CBT-68Ga and CBT-Ga, which warrants 68Ga nanoparticle formation in their MDA-MB-468 tumors, had a tumor/liver ratio 9.1-fold of that of the mice only injected with CBT-68Ga. We envisioned that, by replacing the RVRR substrate of CBT-68Ga with other enzyme-specific ones and using the strategy of intracellular nanoparticle formation, a series of radioactive probes could be developed for more sensitive and precise tumor microPET imaging in the near future.

Keywords: nanoparticle formation; micropet imaging; tumor

Journal Title: Analytical chemistry
Year Published: 2019

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