Pain Signaling by GPCRs and RTKs

Brain L. Schmidt; Francesco De Logu; Romina Nassini; Pierangelo Geppetti; Nigel W. Bunnett

doi:10.1016/j.tips.2025.02.002

Pain Signaling by GPCRs and RTKs

Brain L. Schmidt, Francesco De Logu, Romina Nassini, Pierangelo Geppetti, Nigel W. Bunnett

Research output: Contribution to journal › Review article › peer-review

Abstract

Chronic pain is common and debilitating, yet is inadequately treated by current therapies, which can have life-threatening side effects. Treatments targeting G protein-coupled receptors (GPCRs) and receptor tyrosine kinases (RTKs), key pain mediators, often fail in clinical trials for unknown reasons. Here, we discuss the recent evidence that GPCRs and RTKs generate sustained signals from multiprotein signaling complexes or signalosomes in intracellular compartments to control chronic pain. We evaluate the evidence that selective antagonism of these intracellular signals provides more efficacious and long-lasting pain relief than antagonism of receptors at the surface of cells. We highlight how the identification of coreceptors and molecular scaffolds that underpin pain signaling by multiple receptors has identified new therapeutic targets for chronic pain, surmounting the redundancy of the pain signaling pathway.

Original language	English (US)
Pages (from-to)	372-385
Number of pages	14
Journal	Trends in Pharmacological Sciences
Volume	46
Issue number	4
DOIs	https://doi.org/10.1016/j.tips.2025.02.002
State	Published - Apr 2025

Keywords

analgesia
pain
signal transduction
trafficking

ASJC Scopus subject areas

Toxicology
Pharmacology

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10.1016/j.tips.2025.02.002

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title = "Pain Signaling by GPCRs and RTKs",

abstract = "Chronic pain is common and debilitating, yet is inadequately treated by current therapies, which can have life-threatening side effects. Treatments targeting G protein-coupled receptors (GPCRs) and receptor tyrosine kinases (RTKs), key pain mediators, often fail in clinical trials for unknown reasons. Here, we discuss the recent evidence that GPCRs and RTKs generate sustained signals from multiprotein signaling complexes or signalosomes in intracellular compartments to control chronic pain. We evaluate the evidence that selective antagonism of these intracellular signals provides more efficacious and long-lasting pain relief than antagonism of receptors at the surface of cells. We highlight how the identification of coreceptors and molecular scaffolds that underpin pain signaling by multiple receptors has identified new therapeutic targets for chronic pain, surmounting the redundancy of the pain signaling pathway.",

keywords = "analgesia, pain, signal transduction, trafficking",

author = "Schmidt, {Brain L.} and {De Logu}, Francesco and Romina Nassini and Pierangelo Geppetti and Bunnett, {Nigel W.}",

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T1 - Pain Signaling by GPCRs and RTKs

AU - Schmidt, Brain L.

AU - De Logu, Francesco

AU - Nassini, Romina

AU - Geppetti, Pierangelo

AU - Bunnett, Nigel W.

PY - 2025/4

Y1 - 2025/4

N2 - Chronic pain is common and debilitating, yet is inadequately treated by current therapies, which can have life-threatening side effects. Treatments targeting G protein-coupled receptors (GPCRs) and receptor tyrosine kinases (RTKs), key pain mediators, often fail in clinical trials for unknown reasons. Here, we discuss the recent evidence that GPCRs and RTKs generate sustained signals from multiprotein signaling complexes or signalosomes in intracellular compartments to control chronic pain. We evaluate the evidence that selective antagonism of these intracellular signals provides more efficacious and long-lasting pain relief than antagonism of receptors at the surface of cells. We highlight how the identification of coreceptors and molecular scaffolds that underpin pain signaling by multiple receptors has identified new therapeutic targets for chronic pain, surmounting the redundancy of the pain signaling pathway.

AB - Chronic pain is common and debilitating, yet is inadequately treated by current therapies, which can have life-threatening side effects. Treatments targeting G protein-coupled receptors (GPCRs) and receptor tyrosine kinases (RTKs), key pain mediators, often fail in clinical trials for unknown reasons. Here, we discuss the recent evidence that GPCRs and RTKs generate sustained signals from multiprotein signaling complexes or signalosomes in intracellular compartments to control chronic pain. We evaluate the evidence that selective antagonism of these intracellular signals provides more efficacious and long-lasting pain relief than antagonism of receptors at the surface of cells. We highlight how the identification of coreceptors and molecular scaffolds that underpin pain signaling by multiple receptors has identified new therapeutic targets for chronic pain, surmounting the redundancy of the pain signaling pathway.

KW - analgesia

KW - pain

KW - signal transduction

KW - trafficking

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DO - 10.1016/j.tips.2025.02.002

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SN - 0165-6147

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EP - 385

JO - Trends in Pharmacological Sciences

JF - Trends in Pharmacological Sciences

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Pain Signaling by GPCRs and RTKs

Abstract

Keywords

ASJC Scopus subject areas

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