GPR68, a proton-sensing GPCR, mediates acid-induced visceral nociception

  1. Luke W Paine
  2. Rohit Gupta
  3. James P Higham
  4. Javier Aguilera-Lizarraga
  5. Anne Ritoux
  6. Thomas Pritchard
  7. Samuel Nicholson
  8. James R F Hockley
  9. Tim Raine
  10. Martin Hausmann
  11. Kyle Bednar
  12. Gerhard Rogler
  13. Fraser Welsh
  14. Ewan St John Smith
  15. David C Bulmer
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Abstract

Background & Aims

Localised acidification from immune cell infiltration and heightened glycolysis contributes to colitis pathology by activating acid-sensing receptors such as GPR68, a proton-sensing GPCR expressed on immune and stromal cells. Single-cell RNAseq analysis revealed GPR68 is also expressed in colonic sensory neurons, prompting us to investigate its role in acid-induced colonic nociception.

Methods

Expression of GPR68 in colonic nociceptors and tissue from people with colitis was confirmed by in silico analysis of our RNAseq databases. Its contribution to disease activity was assessed using the acute dextran sulphate sodium (DSS) model of colitis. Acid-evoked sensory signalling was evaluated via colonic afferent recordings and Ca²⁺ imaging in DRG neurons from wild-type and GPR68 -/- mice, supported by pharmacological studies using Ogerin (a GPR68 positive allosteric modulator) and Ogremorphin (a GPR68 antagonist).

Results

RNAseq analysis showed GPR68 is robustly expressed in Trpv1 ⁺ colonic nociceptors and upregulated in tissue from people with inflammatory bowel disease, consistent with reduced disease activity in DSS-treated GPR68 -/- mice. Genetic deletion of GPR68 abolished colonic afferent responses to acid, which were also attenuated by Ogremorphin and enhanced by Ogerin. In Ca²⁺-free buffer, DRG neurons from GPR68 -/- mice or those pre-treated with Ogremorphin showed significantly reduced acid-evoked intracellular Ca²⁺ responses. By contrast the colonic afferent and DRG Ca 2+ response (in Ca 2+ -containing buffer) to capsaicin was comparable between tissue from wild-type and GPR68 -/- mice highlighting the involvement of divergent proton-dependent cellular signalling cascades.

Conclusions

These findings identify GPR68 as a key mediator of acid-induced colonic nociception and highlight its potential as a therapeutic target for the treatment of pain in colitis.

Synopsis

We demonstrate that the proton-sensing receptor GPR68 mediates acid-induced signalling in colonic sensory neurons. Genetic and pharmacological modulation confirms GPR68’s role in visceral nociception and supports its potential as a therapeutic target for pain management in colitis.

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  1. Version published to 10.1101/2025.06.13.659465v1 on bioRxiv