IL-1-dependent enteric gliosis guides intestinal inflammation and dysmotility and modulates macrophage function

Schneider, Reiner; Leven, Patrick; Mallesh, Shilpashree; Breßer, Mona; Schneider, Linda; Mazzotta, Elvio; Fadda, Paolo; Glowka, Tim R.; Vilz, Tim O.; Lingohr, Philipp; Kalff, Jörg C.; Christofi, Fievos L.; Wehner, Sven

doi:10.1038/s42003-022-03772-4

Cited by 23 publications

(39 citation statements)

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“…'Reactive' enteric glial cells are emerging as an important target of investigation in neurogastroenterology and motility for gastrointestinal diseases (Gulbransen & Christofi, 2018;Mazzotta et al, 2020;Ochoa-Cortes et al, 2016;Schneider et al, 2021Schneider et al, , 2022Stoffels et al, 2014). 'Reactive' glia are…”

Section: Discussionmentioning

confidence: 99%

“…The availability of more selective tools to study ET B receptor signalling, including selective drugs such as BQ788 or sarafotoxin, Tg (Ednrb-EGFP)EP59Gsat/Mmucd mice, specific antisera against EGFP, ET-1 and ET B receptor, cell-specific Ca 2+ reporter mice for glia (Sox10 CreERT2 ;GCaMP5g-tdT) or neurons (Wnt1 Cre2 ;GCaMP5g-tdT) to monitor enteric nervous system activation, RiboTag mice, and spatiotemporal imaging of peristalsis, provided definitive ways to investigate ET B receptor signalling in health or disease. To evaluate ET B receptor signalling in 'reactive' glia, we used an established mouse model of postoperative ileus (POI) that is linked to muscularis externa (ME) inflammation and disruption of motility (Schneider et al, 2021(Schneider et al, , 2022Stoffels et al, 2014). ET B receptor signalling in human enteric glia was confirmed by Ca 2+ imaging in glial networks obtained from surgical specimens.…”

Section: What Is the Clinical Significancementioning

confidence: 99%

“…signalling in 'reactive' glia (Bhave et al, 2017;Gulbransen et al, 2012;Liñán-Rico et al, 2016;McClain & Gulbransen, 2017;Schneider et al, 2021;Schneider et al, 2022;Stoffels et al, 2014) is altered after gut inflammation in a well characterized POI mouse model of muscularis externa inflammation induced by surgical intestinal manipulation (IM) (Schneider et al, 2021;Schneider et al, 2022;Stoffels et al, 2014) (Figures S7 and S8). In the POI model, inflammation (Figures S7 and S8) and disruption of motility (slower GI transit) are hallmarks of the disease.…”

Section: Bq788 Amplification Of Excitatory Cholinergic Transmission A...mentioning

confidence: 99%

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BQ788 reveals glial ET_B receptor modulation of neuronal cholinergic and nitrergic pathways to inhibit intestinal motility: Linked to postoperative ileus

Mazzotta

Grants

Villalobos-Hernandez

et al. 2023

British J Pharmacology

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Background and PurposeET‐1 signalling modulates intestinal motility and inflammation, but the role of ET‐1/ETB receptor signalling is poorly understood. Enteric glia modulate normal motility and inflammation. We investigated whether glial ETB signalling regulates neural‐motor pathways of intestinal motility and inflammation.Experimental ApproachWe studied ETB signalling using: ETB drugs (ET‐1, SaTX, BQ788), activity‐dependent stimulation of neurons (high K+‐depolarization, EFS), gliotoxins, Tg (Ednrb‐EGFP)EP59Gsat/Mmucd mice, cell‐specific mRNA in Sox10CreERT2;Rpl22‐HAflx or ChATCre;Rpl22‐HAflx mice, Sox10CreERT2::GCaMP5g‐tdT, Wnt1Cre2::GCaMP5g‐tdT mice, muscle tension recordings, fluid‐induced peristalsis, ET‐1 expression, qPCR, western blots, 3‐D LSM‐immunofluorescence co‐labelling studies in LMMP‐CM and a postoperative ileus (POI) model of intestinal inflammation.Key ResultsIn the muscularis externa ETB receptor is expressed exclusively in glia. ET‐1 is expressed in RiboTag (ChAT)‐neurons, isolated ganglia and intra‐ganglionic varicose‐nerve fibres co‐labelled with peripherin or SP. ET‐1 release provides activity‐dependent glial ETB receptor modulation of Ca2+ waves in neural evoked glial responses. BQ788 reveals amplification of glial and neuronal Ca2+ responses and excitatory cholinergic contractions, sensitive to L‐NAME. Gliotoxins disrupt SaTX‐induced glial‐Ca2+ waves and prevent BQ788 amplification of contractions. The ETB receptor is linked to inhibition of contractions and peristalsis. Inflammation causes glial ETB up‐regulation, SaTX‐hypersensitivity and glial amplification of ETB signalling. In vivo BQ788 (i.p., 1 mg·kg−1) attenuates intestinal inflammation in POI.Conclusion and ImplicationsEnteric glial ET‐1/ETB signalling provides dual modulation of neural‐motor circuits to inhibit motility. It inhibits excitatory cholinergic and stimulates inhibitory nitrergic motor pathways. Amplification of glial ETB receptors is linked to muscularis externa inflammation and possibly pathogenic mechanisms of POI.

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Section: Discussionmentioning

confidence: 99%

Section: What Is the Clinical Significancementioning

confidence: 99%

Section: Bq788 Amplification Of Excitatory Cholinergic Transmission A...mentioning

confidence: 99%

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BQ788 reveals glial ET_B receptor modulation of neuronal cholinergic and nitrergic pathways to inhibit intestinal motility: Linked to postoperative ileus

Mazzotta

Grants

Villalobos-Hernandez

et al. 2023

British J Pharmacology

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Section: Discussionmentioning

confidence: 99%

“…(68) In the gut, gliosis involves enhanced inflammatory signaling in EGC, and it has been reported increasingly in the literature in response to many intestinal disease and injury states like chemotherapy, inflammation, infection and motility disorders. (32,57,(69)(70)(71)(72) This reactive state is associated with the release of many cytokines and glial factors which would have direct interactions with the mucosal barrier, and thus could be an important component to mucosal response to acute injury as seen in this pig model of acute intestinal injury. In keeping with this, when treating injured EGC with glial cell inhibitor fluoroacetate (FA), ischemia-induced upregulation of GFAP, one described marker of the EGC gliosis phenotype, is inhibited.…”

Section: Discussionmentioning

confidence: 99%

Enteric Glial Cell Network Function is Required for Epithelial Barrier Restitution following Intestinal Ischemic Injury in the Early Postnatal Period

Ziegler

Erwin

Caldwell

et al. 2022

Preprint

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Ischemic damage to the intestinal epithelial barrier, such as in necrotizing enterocolitis or small intestinal volvulus, is associated with higher mortality rates in younger patients. We have recently reported a powerful pig model to investigate these age-dependent outcomes in which mucosal barrier restitution is strikingly absent in neonates but can be rescued by direct application of homogenized mucosa from older, juvenile pigs by a yet-undefined mechanism. Within the mucosa, a postnatally developing network of enteric glial cells (EGC) is gaining recognition as a key regulator of the mucosal barrier. Therefore, we hypothesized that the developing EGC network may play an important role in coordinating intestinal barrier repair in neonates. Neonatal and juvenile jejunal mucosa recovering from surgically induced intestinal ischemia was visualized by scanning electron microscopy and the transcriptomic phenotypes were assessed by bulk RNA sequencing. EGC network density and gliosis were examined by gene set enrichment analysis, three-dimensional volume imaging and western blot and its function in regulating epithelial restitution assessed ex vivo in Ussing chamber using the glia-specific inhibitor fluoroacetate, and in vivo by co-culture assay. Here we refine and elaborate our translational model, confirming a neonatal phenotype characterized by a complete lack of coordinated reparative signaling in the mucosal microenvironment. Further, we report important evidence that the subepithelial EGC network changes significantly over the early postnatal period and demonstrate that EGC function in close proximity to wounded intestinal epithelium is critical to intestinal barrier restitution following ischemic injury.

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Glial cell-derived soluble factors increase the metastatic potential of pancreatic adenocarcinoma cells and induce epithelial-to-mesenchymal transition

García-Reyes

Kuzmanov

Schneider

et al. 2023

J Cancer Res Clin Oncol

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Background Pancreatic ductal adenocarcinoma (PDAC) is one of the most aggressive types of cancer, characterized by the spreading of highly metastatic cancer cells, including invasion into surrounding nerves and perineural spaces. Nerves, in turn, can invade the tumor tissue and, through the secretion of neurotrophic factors, chemokines, and cytokines, contribute to PDAC progression. However, the contribution of the nerve-associated glial cells to PDAC progression is not well characterized. Methods Two murine PDAC cell lines were cultured with the conditioned media (CM) of primary enteric glial cells or IMS32 Schwann cells (SCs). Different properties of PDAC cells, such as invasiveness, migratory capacity, and resistance to gemcitabine, were measured by RT-qPCR, microscopy, and MTT assays. Using a neuronal cell line, the observed effects were confirmed to be specific to the glial lineage. Results Compared to the control medium, PDAC cells in the glial cell-conditioned medium showed increased invasiveness and migratory capacity. These cells showed reduced E-cadherin and increased N-cadherin and Vimentin levels, all markers of epithelial–mesenchymal transition (EMT). Primary enteric glial cell CM inhibited the proliferation of PDAC cells but preserved their viability, upregulated transcription factor Snail, and increased their resistance to gemcitabine. The conditioned medium generated from the IMS32 SCs produced comparable results. Conclusion Our data suggest that glial cells can increase the metastatic potential of PDAC cells by increasing their migratory capacity and inducing epithelial-to-mesenchymal transition, a re-programming that many solid tumors use to undergo metastasis. Glial cell-conditioned medium also increased the chemoresistance of PDAC cells. These findings may have implications for future therapeutic strategies, such as targeting glial cell-derived factor signaling in PDAC.

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IL-1-dependent enteric gliosis guides intestinal inflammation and dysmotility and modulates macrophage function

Cited by 23 publications

References 62 publications

BQ788 reveals glial ET_B receptor modulation of neuronal cholinergic and nitrergic pathways to inhibit intestinal motility: Linked to postoperative ileus

BQ788 reveals glial ET_B receptor modulation of neuronal cholinergic and nitrergic pathways to inhibit intestinal motility: Linked to postoperative ileus

Enteric Glial Cell Network Function is Required for Epithelial Barrier Restitution following Intestinal Ischemic Injury in the Early Postnatal Period

Glial cell-derived soluble factors increase the metastatic potential of pancreatic adenocarcinoma cells and induce epithelial-to-mesenchymal transition

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IL-1-dependent enteric gliosis guides intestinal inflammation and dysmotility and modulates macrophage function

Cited by 23 publications

References 62 publications

BQ788 reveals glial ETB receptor modulation of neuronal cholinergic and nitrergic pathways to inhibit intestinal motility: Linked to postoperative ileus

BQ788 reveals glial ETB receptor modulation of neuronal cholinergic and nitrergic pathways to inhibit intestinal motility: Linked to postoperative ileus

Enteric Glial Cell Network Function is Required for Epithelial Barrier Restitution following Intestinal Ischemic Injury in the Early Postnatal Period

Glial cell-derived soluble factors increase the metastatic potential of pancreatic adenocarcinoma cells and induce epithelial-to-mesenchymal transition

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BQ788 reveals glial ET_B receptor modulation of neuronal cholinergic and nitrergic pathways to inhibit intestinal motility: Linked to postoperative ileus

BQ788 reveals glial ET_B receptor modulation of neuronal cholinergic and nitrergic pathways to inhibit intestinal motility: Linked to postoperative ileus