| Literature DB >> 26602277 |
Izzat T Raheem1, John D Schreier1, Joy Fuerst2, Liza Gantert3, Eric D Hostetler3, Sarah Huszar4, Aniket Joshi3, Monika Kandebo5, Somang H Kim6, Jing Li7, Bennett Ma6, Georgia McGaughey8, Sujata Sharma9, William D Shipe1, Jason Uslaner4, George H Vandeveer1, Youwei Yan9, John J Renger5, Sean M Smith5, Paul J Coleman1, Christopher D Cox1.
Abstract
Herein, we present the identification of a novel class of pyrazolopyrimidine phosphodiesterase 10A (PDE10A) inhibitors. Beginning with a lead molecule (1) identified through a fragment-based drug discovery (FBDD) effort, lead optimization was enabled by rational design, X-ray crystallography, metabolic and off-target profiling, and fragment scaffold-hopping. We highlight the discovery of PyP-1, a potent, highly selective, and orally bioavailable pyrazolopyrimidine inhibitor of PDE10A. PyP-1 exhibits sub-nanomolar potency (PDE10A Ki=0.23nM), excellent pharmacokinetic (PK) and physicochemical properties, and a clean off-target profile. It displays dose-dependent efficacy in numerous pharmacodynamic (PD) assays that measure potential for anti-psychotic activity and cognitive improvement. PyP-1 also has a clean preclinical profile with respect to cataleptic potential in rats, prolactin secretion, and weight gain, common adverse events associated with currently marketed therapeutics. Further, PyP-1 displays in vivo preclinical target engagement as measured by PET enzyme occupancy in concert with [(11)C]MK-8193, a novel PDE10A PET tracer.Entities:
Keywords: Antipsychotic activity; Cognitive improvement; Fragment-based drug discovery; Phosphodiesterase 10A; Positron emission tomography; Pyrazolopyrimidine; Rational design; Schizophrenia
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Year: 2015 PMID: 26602277 DOI: 10.1016/j.bmcl.2015.11.013
Source DB: PubMed Journal: Bioorg Med Chem Lett ISSN: 0960-894X Impact factor: 2.823