Intestinal neuropod cell GUCY2C regulates visceral pain
Joshua R. Barton, … , Manuel Covarrubias, Scott A. Waldman
Joshua R. Barton, … , Manuel Covarrubias, Scott A. Waldman
Published December 22, 2022
Citation Information: J Clin Invest. 2023;133(4):e165578. https://doi.org/10.1172/JCI165578.
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Research Article Gastroenterology Neuroscience

Intestinal neuropod cell GUCY2C regulates visceral pain

Abstract

Visceral pain (VP) is a global problem with complex etiologies and limited therapeutic options. Guanylyl cyclase C (GUCY2C), an intestinal receptor producing cyclic GMP(cGMP), which regulates luminal fluid secretion, has emerged as a therapeutic target for VP. Indeed, FDA-approved GUCY2C agonists ameliorate VP in patients with chronic constipation syndromes, although analgesic mechanisms remain obscure. Here, we revealed that intestinal GUCY2C was selectively enriched in neuropod cells, a type of enteroendocrine cell that synapses with submucosal neurons in mice and humans. GUCY2Chi neuropod cells associated with cocultured dorsal root ganglia neurons and induced hyperexcitability, reducing the rheobase and increasing the resulting number of evoked action potentials. Conversely, the GUCY2C agonist linaclotide eliminated neuronal hyperexcitability produced by GUCY2C-sufficient — but not GUCY2C-deficient — neuropod cells, an effect independent of bulk epithelial cells or extracellular cGMP. Genetic elimination of intestinal GUCY2C amplified nociceptive signaling in VP that was comparable with chemically induced VP but refractory to linaclotide. Importantly, eliminating GUCY2C selectively in neuropod cells also increased nociceptive signaling and VP that was refractory to linaclotide. In the context of loss of GUCY2C hormones in patients with VP, these observations suggest a specific role for neuropod GUCY2C signaling in the pathophysiology and treatment of these pain syndromes.

Authors

Joshua R. Barton, Annie K. Londregan, Tyler D. Alexander, Ariana A. Entezari, Shely Bar-Ad, Lan Cheng, Angelo C. Lepore, Adam E. Snook, Manuel Covarrubias, Scott A. Waldman

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Figure 1

GUCY2C is enriched in a subset of intestinal cells.

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GUCY2C is enriched in a subset of intestinal cells. (A and B) Immunofluo...
(A and B) Immunofluorescence of mouse jejunum (A) or human duodenum (B) reveals intestinal cells with increased GUCY2C expression and basal pseudopods (arrows). White dashed lines delineate intestinal epithelium. (C and D) Live images of GUCY2C-GFP reporter mouse show GFP expression throughout the intestine, punctuated with brightly fluorescent cells with basal pseudopods (arrows) in freshly dissected intestine (C) and intestinal organoids (D). (E) FACS of dissociated GUCY2C-GFP mouse intestinal epithelium (right) compared with nonfluorescent intestine (left) reveals a small population of cells with increased GFP fluorescence intensity (GFP High) (representative of n = 3). (F) GUCY2C-GFPhi cells in the GUCY2C-GFP reporter mouse have increased GUCY2C expression, as shown by immunofluorescence. (G) GFPhi cells are enriched in GUCY2C transcripts compared with bulk intestinal epithelial cells (20,000 cells/sample, 2 samples/mouse, n = 3 mice). (H) The GUCY2C agonist linaclotide induces cGMP production by sorted GFPhi cells (10,000 cells/sample, 2 samples /mouse, n = 3). Scale bars: 25 μm (Merge), 100 μm (Swiss Roll). Statistics calculated using 2-way ANOVA with Tukey’s multiple comparisons test.