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Evaluation of G protein bias and β-arrestin 2 signaling in opioid-induced respiratory depression

Jordan T. Bateman, Erica S. Levitt

2021American Journal of Physiology-Cell Physiology19 citationsDOIOpen Access PDF

Abstract

Respiratory depression is a potentially fatal side effect of opioid analgesics and a major limitation to their use. G protein-biased opioid agonists have been proposed as "safer" analgesics with less respiratory depression. These agonists are biased to activate G proteins rather than β-arrestin signaling. Respiratory depression has been shown to correlate with both G protein bias and intrinsic efficacy, and recent work has refuted the role of β-arrestin signaling in opioid-induced respiratory depression. In addition, there is substantial evidence that G proteins do, in fact, mediate respiratory depression by actions in respiratory-controlling brainstem neurons. Based on these studies, we provide the perspective that protection from respiratory depression displayed by newly developed G protein-biased agonists is due to factors other than G protein versus arrestin bias.

Topics & Concepts

ArrestinRespiratory systemDepression (economics)OpioidPsychologyInternal medicineSignal transductionMedicineBiologyCell biologyReceptorG protein-coupled receptorMacroeconomicsEconomicsReceptor Mechanisms and SignalingNeuroscience of respiration and sleepNeuropeptides and Animal Physiology
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