Pharmacology of JNJ-28583113: A novel TRPM2 antagonist

TRPM2型 药理学 瞬时受体电位通道 离体 敌手 小胶质细胞 体内 化学 受体 体外 生物 炎症 生物化学 免疫学 生物技术
作者
Lawrence Fourgeaud,Curt A. Dvorak,Malika Faouzi,John G. Starkus,Sunil Sahdeo,Qi Wang,Brian Lord,Heather Coate,Natalie Taylor,Yingbo He,Na Qin,Alan Wickenden,Nicholas I. Carruthers,Timothy W. Lovenberg,Reinhold Penner,Anindya Bhattacharya
出处
期刊:European Journal of Pharmacology [Elsevier BV]
卷期号:853: 299-307 被引量:34
标识
DOI:10.1016/j.ejphar.2019.03.043
摘要

Transient receptor potential melastatin type 2 (TRPM2) is a cation channel activated by free intracellular ADP-ribose and reactive oxygen species. TRPM2 signaling has been linked to the pathophysiology of CNS disorders such as neuropathic pain, bipolar disorder and Alzheimer's disease. In this manuscript, we describe the discovery of JNJ-28583113, a potent brain penetrant TRPM2 antagonist. Ca2+ flux assays in cells overexpressing TRPM2 and electrophysiological recordings were used to test the pharmacology of JNJ-28583113. JNJ-28583113 was assayed in vitro on GSK-3 phosphorylation levels, cell death, cytokine release in microglia and unbiased morphological phenotypic analysis. Finally, we dosed animals to evaluate its pharmacokinetic properties. Our results showed that JNJ-28583113 is a potent (126 ± 0.5 nM) TRPM2 antagonist. Blocking TRPM2 caused phosphorylation of GSK3α and β subunits. JNJ-28583113 also protected cells from oxidative stress induced cell death as well as morphological changes induced by non-cytotoxic concentrations of H2O2. In addition, inhibiting TRPM2 blunted cytokine release in response to pro-inflammatory stimuli in microglia. Lastly, we showed that JNJ-28583113 was brain penetrant but not suitable for systemic dosing as it was rapidly metabolized in vivo. While the in-vitro pharmacology of JNJ-28583113 is the best in class, its in-vivo properties would need optimization to assist in further probing key roles of TRPM2 in CNS pathophysiology.
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