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Literature DB >> 29149605

Bias Factor and Therapeutic Window Correlate to Predict Safer Opioid Analgesics.

Cullen L Schmid¹, Nicole M Kennedy², Nicolette C Ross³, Kimberly M Lovell³, Zhizhou Yue², Jenny Morgenweck¹, Michael D Cameron¹, Thomas D Bannister², Laura M Bohn⁴.

Abstract

Biased agonism has been proposed as a means to separate desirable and adverse drug responses downstream of G protein-coupled receptor (GPCR) targets. Herein, we describe structural features of a series of mu-opioid-receptor (MOR)-selective agonists that preferentially activate receptors to couple to G proteins or to recruit βarrestin proteins. By comparing relative bias for MOR-mediated signaling in each pathway, we demonstrate a strong correlation between the respiratory suppression/antinociception therapeutic window in a series of compounds spanning a wide range of signaling bias. We find that βarrestin-biased compounds, such as fentanyl, are more likely to induce respiratory suppression at weak analgesic doses, while G protein signaling bias broadens the therapeutic window, allowing for antinociception in the absence of respiratory suppression.

Entities: CellLine Chemical Disease Gene Species

Keywords: G protein-coupled receptor (GPCR); biased agonism; fentanyl; functional selectivity; morphine; mu opioid receptor; pain; respiration; side effects; βarrestin

Mesh：

Substances：

Year: 2017 PMID： 29149605 PMCID： PMC5731250 DOI： 10.1016/j.cell.2017.10.035

Source DB: PubMed Journal: Cell ISSN： 0092-8674 Impact factor: 41.582

33 in total

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3. A simple method for quantifying functional selectivity and agonist bias.

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6. Bezitramide (R 4845), a new potent and orally long-acting analgesic compound.

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150 in total

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Authors: S Stevens Negus; Megan J Moerke
Journal: Peptides Date: 2018-11-01 Impact factor: 3.750

2. Biased agonists of the chemokine receptor CXCR3 differentially control chemotaxis and inflammation.

Authors: Jeffrey S Smith; Lowell T Nicholson; Jutamas Suwanpradid; Rachel A Glenn; Nicole M Knape; Priya Alagesan; Jaimee N Gundry; Thomas S Wehrman; Amber Reck Atwater; Michael D Gunn; Amanda S MacLeod; Sudarshan Rajagopal
Journal: Sci Signal Date: 2018-11-06 Impact factor: 8.192

3. Molecular mechanism of biased signaling in a prototypical G protein-coupled receptor.

Authors: Carl-Mikael Suomivuori; Naomi R Latorraca; Laura M Wingler; Stephan Eismann; Matthew C King; Alissa L W Kleinhenz; Meredith A Skiba; Dean P Staus; Andrew C Kruse; Robert J Lefkowitz; Ron O Dror
Journal: Science Date: 2020-02-21 Impact factor: 47.728

Review 4. A Biased View of μ-Opioid Receptors?

Authors: Alexandra E Conibear; Eamonn Kelly
Journal: Mol Pharmacol Date: 2019-06-07 Impact factor: 4.436

5. Functional characterization of a novel opioid, PZM21, and its effects on the behavioural responses to morphine.

Authors: Lucja Kudla; Ryszard Bugno; Urszula Skupio; Lucja Wiktorowska; Wojciech Solecki; Adam Wojtas; Krystyna Golembiowska; Ferenc Zádor; Sándor Benyhe; Szymon Buda; Wioletta Makuch; Barbara Przewlocka; Andrzej J Bojarski; Ryszard Przewlocki
Journal: Br J Pharmacol Date: 2019-12-08 Impact factor: 8.739

6. The δ-opioid receptor positive allosteric modulator BMS 986187 is a G-protein-biased allosteric agonist.

Authors: M Alexander Stanczyk; Kathryn E Livingston; Louise Chang; Zara Y Weinberg; Manojkumar A Puthenveedu; John R Traynor
Journal: Br J Pharmacol Date: 2019-04-14 Impact factor: 8.739

7. Opioid-galanin receptor heteromers mediate the dopaminergic effects of opioids.

Authors: Ning-Sheng Cai; César Quiroz; Jordi Bonaventura; Alessandro Bonifazi; Thomas O Cole; Julia Purks; Amy S Billing; Ebonie Massey; Michael Wagner; Eric D Wish; Xavier Guitart; William Rea; Sherry Lam; Estefanía Moreno; Verònica Casadó-Anguera; Aaron D Greenblatt; Arthur E Jacobson; Kenner C Rice; Vicent Casadó; Amy H Newman; John W Winkelman; Michael Michaelides; Eric Weintraub; Nora D Volkow; Annabelle M Belcher; Sergi Ferré
Journal: J Clin Invest Date: 2019-03-26 Impact factor: 14.808