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Literature DB >> 35738565

Characterization of Pyrrolidinyl-hexahydro-pyranopiperazines as a Novel Kappa Opioid Receptor Agonist Scaffold.

Brian Reed¹, Michael Miller², Mayako Michino², Eduardo R Butelman³, Ariel Ben-Ezra³, Philip Pikus³, Michelle Morochnik³, Yuli Kim³, Amy Ripka⁴, Joseph Vacca⁵, Mary Jeanne Kreek³.

Abstract

The kappa agonist structure-activity relationship around the novel, pyrrolidinyl substituted pyranopiperazine scaffold was developed. More specifically, the dichloroPhenylAcetamide-Pyrrolidinyl-PyranoPiperazine (PAPPP) core A was the focus of our work. The modulation of kappa receptor potency/G-protein activation and arrestin recruitment with respect to changes of the piperazine R group in A was demonstrated. Reduced β2-arrestin recruitment and differential G-protein bias were observed for select analogues. To better understand the subtlety in receptor signaling, analogues were profiled as the resolved enantiomers. To determine in vivo target engagement, a subset of compounds was tested in mice for stimulation of serum prolactin, a neuroendocrine biomarker of KOR-agonist effects. Additional in vivo characterization included measurement of potential unwanted effects of kappa receptor activation such as sedation. These studies demonstrate a novel kappa receptor agonist scaffold with potential for G-protein signaling bias to probe in vivo pharmacology.

Entities: Chemical

Keywords: biased agonist; kappa agonist; kappa receptor; opioid receptor

Mesh：

Substances：

Year: 2022 PMID： 35738565 PMCID： PMC9266631 DOI： 10.1021/acschemneuro.2c00258

Source DB: PubMed Journal: ACS Chem Neurosci ISSN： 1948-7193 Impact factor: 5.780

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