Yuhpyng L. Chen

Concentration-Dependent Modulation of Amyloid-β in Vivo and in Vitro Using the γ-Secretase Inhibitor, LY-450139

LY-450139 is a γ-secretase inhibitor shown to have efficacy in multiple cellular and animal models. Paradoxically, robust elevations of plasma amyloid-β (Aβ) have been reported in dogs and humans after administration of subefficacious doses. The present study sought to further evaluate Aβ responses to LY-450139 in the guinea pig, a nontransgenic model that has an Aβ sequence identical to that of human. Male guinea pigs were treated with LY-450139 (0.2–60 mg/kg), and brain, cerebrospinal fluid, and plasma Aβ levels were characterized at 1, 3, 6, 9, and 14 h postdose. Low doses significantly elevated plasma Aβ levels at early time points, with return to baseline within hours. Higher doses inhibited Aβ levels in all compartments at early time points, but elevated plasma Aβ levels at later time points. To determine whether this phenomenon occurs under steady-state drug exposure, guinea pigs were implanted with subcutaneous minipumps delivering LY-450139 (0.3–30 mg/kg/day) for 5 days. Plasma Aβ was significantly inhibited at 10–30 mg/kg/day, but significantly elevated at 1 mg/kg/day. To further understand the mechanism of Aβ elevation by LY-450139, H4 cells overexpressing the Swedish mutant of amyloid-precursor protein and a mouse embryonic stem cell-derived neuronal cell line were studied. In both cellular models, elevated levels of secreted Aβ were observed at subefficacious concentrations, whereas dose-responsive inhibition was observed at higher concentrations. These results suggest that LY-450139 modulates the γ-secretase complex, eliciting Aβ lowering at high concentrations but Aβ elevation at low concentrations.

2-aryloxy-4-alkylaminopyridines: discovery of novel corticotropin-releasing factor 1 antagonists.

An orally active clinical candidate of corticotropin-releasing factor 1 (CRF 1) antagonist 1 showed a significant positive food effect in dog and human after oral administration. Efforts to address the food effect issue led us to explore and discover compounds in series 2 as orally active CRF 1 receptor antagonists, in which some compounds showed improved physicochemical properties while retaining desired pharmacological properties. Compound 3a (CP-376395) was selected for further development, due not only to its reduced food effects but also its greater efficacy in CNS models. Compound 3a was advanced to the clinic. The synthesis of representative potential candidates and their in vitro, ex vivo, and in vivo data are described.

Synthesis of a potent β-lactamase inhibitor-1,1-dioxo-6-(2-pyridyl)methylenepenicillanic acid and its reaction with sodium methoxide

Abstract 1,1-Dioxo-6-(2-pyridyl)methylenepenicillanic acid ( 6 ) was prepared and found to be a potent β-lactamase inhibitor. Its reaction with sodium methoxide was studied to provide insight into its mechanism of enzyme inactivation.

Vinyl protecting group for benzimidazole nitrogen: Synthesis of benzimidazole-penam alcohol

Abstract Use of the vinyl moiety as a protecting group for benzimidazole nitrogen in the synthesis of benzimidazole 2-carboxaldehyde is described. The protected carboxaldehyde is an intermediate in the synthesis of 6-(2-benzimidazole)hydroxymethyl penicillanic acid (1). Deprotection is achieved by ozonolysis.

Kinase domain inhibition of leucine rich repeat kinase 2 (LRRK2) using a [1,2,4]triazolo[4,3-b]pyridazine scaffold.

Leucine rich repeat kinase 2 (LRRK2) has been genetically linked to Parkinsons disease (PD). The most common mutant, G2019S, increases kinase activity, thus LRRK2 kinase inhibitors are potentially useful in the treatment of PD. We herein disclose the structure, potential ligand-protein binding interactions, and pharmacological profiling of potent and highly selective kinase inhibitors based on a triazolopyridazine chemical scaffold.

Total synthesis of an optically active 8-carba-physostigmine analog: a potent acetylcholinesterase inhibitor

Abstract Syntheses of 8-carba-physostigmine enantiomers 2a and 2b via optically active intermediates 9a and 9b are described. The key synthetic intermediate 9 was prepared via a [2 + 2] cycloaddition of indene 4 and dichloroketene, followed by Beckmann rearrangement, reduction and resolution.