Colin Chinn scite author profile

Using a novel physiologically relevant in vitro human whole blood neutrophil shape change assay, an aminopyrazine series of selective PI3Kγ inhibitors was identified and prioritized for further optimization. Severe solubility limitations associated with the series leading to low oral bioavailability and poor exposures, especially at higher doses, were overcome by moving to an aminopyridine core. Compound 33, with the optimal balance of on-target activity, selectivity, and pharmacokinetic parameters, progressed into in vivo studies and demonstrated good efficacy (10 mg/kg) in a rat model of airway inflammation. Sufficient exposures were achieved at high doses to support toxicological studies, where unexpected inflammatory cell infiltrates in cardiovascular tissue prevented further compound development.

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Medical and Mental Health Preparations: 3rd Battalion, 5th Marines (3/5) Return

Faison¹,

Chinn²,

Regner³

et al. 2011

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Colin Chinn

Acute Hepatitis After Ingestion of Herbs

Development of autotaxin inhibitors: A series of zinc binding triazoles

Excretion and Distribution of Thiazesim-14C with Its Biotransformation In Vivo and In Vitro

Discovery and Toxicological Profiling of Aminopyridines as Orally Bioavailable Selective Inhibitors of PI3-Kinase γ

Medical and Mental Health Preparations: 3rd Battalion, 5th Marines (3/5) Return

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