Publication | Closed Access
Novel Matrix Metalloproteinase Inhibitor [18F]Marimastat-Aryltrifluoroborate as a Probe for <i>In vivo</i> Positron Emission Tomography Imaging in Cancer
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Citations
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References
2010
Year
EngineeringOncologic ImagingTumor BiologyPositron Emission TomographyOncologyNoncovalent Mmp InhibitorMatrix MetalloproteinasesTheranosticsAnti-cancer AgentRadiation OncologyMolecular ImagingNuclear MedicineCancer ResearchRadiologyActive Transmembrane Mmp14Tumor TargetingRadiologic ImagingPharmacologyTumor MicroenvironmentBiomolecular EngineeringDrug TargetingBiomedical ImagingMedicine
Matrix metalloproteinases (MMP), strongly associated pathogenic markers of cancer, have undergone extensive drug development programs. Marimastat, a noncovalent MMP inhibitor, was conjugated with FITC to label cellular metalloproteinase cancer targets in MDA-MB-231 cells in vitro. Punctate localization of active transmembrane MMP14 was observed. For molecular-targeted positron emission tomography imaging of syngeneic 67NR murine mammary carcinoma in vivo, marimastat was (18)F-labeled using a shelf-stable arylboronic ester conjugate as a captor for aqueous [(18)F]fluoride in a novel, rapid one-step reaction at ambient temperature. [(18)F]Marimastat-aryltrifluoroborate localized to the tumors, with labeling being blocked in control animals first loaded with >10-fold excess unlabeled marimastat. The labeled drug cleared primarily via the hepatobiliary and gastrointestinal tract, with multiple animals imaged in independent experiments, confirming the ease of this new labeling strategy.
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