Literature DB >> 31812677

Development and preclinical pharmacology of a novel dCK inhibitor, DI-87.

Soumya Poddar1, Edmund V Capparelli2, Ethan W Rosser3, Raymond M Gipson4, Liu Wei1, Thuc Le1, Michael E Jung5, Caius Radu1, Mina Nikanjam6.   

Abstract

BACKGROUND: Deoxycytidine kinase (dCK) is an essential enzyme for production of nucleotides via the salvage pathway; DI-87 is a novel dCK inhibitor in preclinical development for use in anticancer therapy. The current study utilizes PET imaging to evaluate PK-PD relationships and to determine optimal dosing of the drug.
METHODS: NSG mice bearing CEM tumors had plasma and tumor PK assessed using mass spectrometry following oral administration of DI-87. dCK inhibition was assessed after a single dose of oral DI-87 followed by a [18F]CFA PET probe and PET imaging. Tumor growth inhibition was assessed by orally administering DI-87 with concurrent intraperitoneal thymidine.
RESULTS: DI-87 had an in vitro EC50 of 10.2 nM with low protein binding. Peak DI-87 concentrations were observed between 1-3 h and 3-9 h in plasma and tumor, respectively, with tumor concentrations less than one third of plasma. Full dCK inhibition, as evaluated by PET imaging, was observed as early as 3 h following 25 mg/kg dosing and was maintained for 12 h, with full recovery of enzyme activity after 36 h. When DI-87 was administered as repeated doses in combination with thymidine, full dCK inhibition was maintained at 12 h (25 mg/kg twice daily dose) and led to maximal tumor growth inhibition.
CONCLUSIONS: DI-87 is a promising new compound for use in combination therapy against tumors expressing dCK. Utilizing a [18F]CFA PET probe targeting the pathway of interest allowed for efficient and accurate identification of the optimal dose for growth inhibition.
Copyright © 2019 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  DI-87; Deoxycytidine kinase; PET scan; Pharmacodynamics; Pharmacokinetics; Preclinical

Mesh:

Substances:

Year:  2019        PMID: 31812677      PMCID: PMC6981055          DOI: 10.1016/j.bcp.2019.113742

Source DB:  PubMed          Journal:  Biochem Pharmacol        ISSN: 0006-2952            Impact factor:   5.858


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