Endosomal signaling of the receptor for calcitonin gene-related peptide mediates pain transmission

Yarwood, Rebecca; Imlach, Wendy L.; Lieu, Tina Marie; Veldhuis, Nicholas A.; Jensen, Dane D.; Herenbrink, Carmen Klein; Aurelio, Luigi; Cai, Zhijian; Christie, MacDonald J.; Poole, Daniel P.; Porter, Christopher John; McLean, Peter G.; Hicks, Gareth A.; Geppetti, Pierangelo; Halls, Michelle L.; Canals, Meritxell; Bunnett, Nigel W.

doi:10.1073/pnas.1706656114

Cited by 139 publications

(183 citation statements)

References 29 publications

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“…Another is to deliberately exploit the potential of conformationally selective nanobodies to block GPCR signaling reactions, specifically localizing them to a defined target membrane using chemical recruitment tools and assessing effect on the cellular response . A third approach, which may also have therapeutic potential with further development, is to generate antagonist ligands that accumulate in endosomes to inhibit activation in this compartment selectively …”

Section: G Protein Signaling From Endosomes: a Continuation Or New Bementioning

confidence: 99%

“…13,37 Over the last decade, however, the hypothesis that GPCRs can initiate G protein-coupled signaling from endosomes as well as the plasma membrane has gained considerable experimental support. [38][39][40][41][42][43][44][45][46][47][48][49][50][51][52][53][54][55] Evidence for GPCR-G protein signaling from endosomes. Broadly considered, four experimental approaches have produced evidence supporting endosomal GPCR-G protein signaling.…”

mentioning

confidence: 99%

“…48,54 In a third approach, GPCR endocytosis was inhibited using genetic or chemical manipulations; endocytic blockade was found to reduce the strength and/or duration of downstream cellular responses. 39,40,42,45,46,49,50 In a fourth approach, biosensors derived from single-domain antibodies (nanobodies) were used to localize active-conformation GPCRs as well as detect conformational activation of G protein;…”

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confidence: 99%

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When trafficking and signaling mix: How subcellular location shapes G protein‐coupled receptor activation of heterotrimeric G proteins

Lobingier

Zastrow

2019

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G protein‐coupled receptors (GPCRs) physically connect extracellular information with intracellular signal propagation. Membrane trafficking plays a supportive role by “bookending” signaling events: movement through the secretory pathway delivers GPCRs to the cell surface where receptors can sample the extracellular environment, while endocytosis and endolysosomal membrane trafficking provide a versatile system to titrate cellular signaling potential and maintain homeostatic control. Recent evidence suggests that, in addition to these important effects, GPCR trafficking actively shapes the cellular signaling response by altering the location and timing of specific receptor‐mediated signaling reactions. Here, we review key experimental evidence underlying this expanding view, focused on GPCR signaling mediated through activation of heterotrimeric G proteins located in the cytoplasm. We then discuss lingering and emerging questions regarding the interface between GPCR signaling and trafficking.

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Section: G Protein Signaling From Endosomes: a Continuation Or New Bementioning

confidence: 99%

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confidence: 99%

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confidence: 99%

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When trafficking and signaling mix: How subcellular location shapes G protein‐coupled receptor activation of heterotrimeric G proteins

Lobingier

Zastrow

2019

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“…Recent studies have revealed the importance of the texture of the initiated intracellular signal in controlling unique physiological outcomes, including both spatial (i.e., subcellular compartmentalisation of the signal) and temporal (i.e., changes in the signal over time) properties (Calebiro et al, ; DeFea, ; Godbole, Lyga, Lohse, & Calebiro, ; Irannejad et al, ; Irannejad et al, ; Kotowski, Hopf, Seif, Bonci, & von Zastrow, ; Mullershausen et al, ; Nikolaev, Bünemann, Schmitteckert, Lohse, & Engelhardt, ; Tsvetanova & von Zastrow, ; Wehbi et al, ). These shifts in the way we understand canonical GPCR activation and downstream signalling are already opening exciting new avenues for drug discovery (Jensen et al, ; Jimenez‐Vargas et al, ; Yarwood et al, ).…”

Section: G‐protein Coupled Receptorsmentioning

confidence: 99%

“…Recent advances in the understanding of compartmentalised GPCR signalling have illustrated the importance of receptor location (within different plasma membrane domains or within different subcellular compartments) for the control of distinct signalling outcomes (Halls et al, 2016;Jensen et al, 2017;Jimenez-Vargas et al, 2018;Stoeber et al, 2018;Tsvetanova & von Zastrow, 2014;Yarwood et al, 2017). Cellular context also appears to be very important in order for GPCRs to respond to ultra-low concentrations of ligand ( Figure 1).…”

Section: Other Gpcrs Can Generate Ultra-sensitive Cellular Responsesmentioning

confidence: 99%

Signalling in response to sub‐picomolar concentrations of active compounds: Pushing the boundaries of GPCR sensitivity

Civciristov

Halls

2019

British J Pharmacology

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There is evidence for ultra‐sensitive responses to active compounds at concentrations below picomolar levels by proteins and receptors found in species ranging from bacteria to mammals. We have recently shown that such ultra‐sensitivity is also demonstrated by a wide range of prototypical GPCRs, and we have determined the molecular mechanisms behind these responses for three family A GPCRs: the relaxin receptor, RXFP1; the β2‐adrenoceptor; and the M3 muscarinic ACh receptor. Interestingly, there are reports of similar ultra‐sensitivity by more than 15 human GPCR families, in addition to other human receptors and channels. These occur through a diverse range of signalling pathways and produce modulation of important physiological processes, including neuronal transmission, chemotaxis, gene transcription, protein/ion uptake and secretion, muscle contraction and relaxation, and phagocytosis. Here, we summarise the accumulating evidence of ultra‐sensitive receptor signalling to show that this is a common, though currently underappreciated, property of GPCRs. Linked Articles This article is part of a themed section on Adrenoceptors—New Roles for Old Players. To view the other articles in this section visit http://onlinelibrary.wiley.com/doi/10.1111/bph.v176.14/issuetoc

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GPCRs at Endosomes: Sorting, Signaling, and Recycling

Irannejad¹,

Lobingier²

2022

GPCRs as Therapeutic Targets

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Endosomal signaling of the receptor for calcitonin gene-related peptide mediates pain transmission

Cited by 139 publications

References 29 publications

When trafficking and signaling mix: How subcellular location shapes G protein‐coupled receptor activation of heterotrimeric G proteins

When trafficking and signaling mix: How subcellular location shapes G protein‐coupled receptor activation of heterotrimeric G proteins

Signalling in response to sub‐picomolar concentrations of active compounds: Pushing the boundaries of GPCR sensitivity

GPCRs at Endosomes: Sorting, Signaling, and Recycling

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