Gut microbiota dysbiosis affects intestinal sensitivity through epithelium-to-neuron signaling: novel insights from a colon organoid-based model to improve visceral pain therapy

Francesco Margiotta; Elena Lucarini; Alessandra Toti; Lorenzo Curti; Alessio Masi; Tommaso Mello; Gwenaelle Le Gall; Gianluca Mattei; Alberto Magi; David Vauzour; Guido Mannaioni; Lorenzo Di Cesare Mannelli; Carla Ghelardini

doi:10.1080/19490976.2025.2547029

Gut microbiota dysbiosis affects intestinal sensitivity through epithelium-to-neuron signaling: novel insights from a colon organoid-based model to improve visceral pain therapy

Francesco Margiotta, Elena Lucarini, Alessandra Toti, Lorenzo Curti, Alessio Masi, Tommaso Mello, Gwenaelle Le Gall, Gianluca Mattei, Alberto Magi, David Vauzour, Guido Mannaioni, Lorenzo Di Cesare Mannelli, Carla Ghelardini

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Abstract

Chronic gastrointestinal pain is a hallmark of most intestinal pathologies, yet effective treatments remain elusive given the complexity of the underlying mechanisms. Aiming to investigate the intestinal epithelium contribution to visceral pain modulation in dysbiosis context, we first demonstrated that intracolonic instillation of microbe-free fecal supernatants from mice with post-inflammatory dysbiosis induced by dextran sodium sulfate (FSDSS) provokes visceral hypersensitivity in recipient mice. Epithelium involvement in the response to FSDSS was analyzed through a novel in vitro approach comprising murine epithelial colon organoids and primary dorsal root ganglia (DRG) neurons. FSDSS treatment induced growth and metabolic impairment in colon organoids, which revealed a dysbiosis-driven epithelial dysfunction. Notably, the combination of FSDSS and conditioned medium from FSDSS-treated colon organoids induced an increase in DRG neuron intrinsic excitability, along with greater immunoreactivity to c-Fos and calcitonin-gene related peptide, implicating an integrated role of both microbial and epithelial products in visceral sensitivity regulation. By investigating the underlying signaling, metabolomic analysis revealed reduced levels of short chain fatty acids in FSDSS, such as butyrate, acetate, valerate, and propionate. Moreover, transcriptomic analysis of FSDSS-treated colon organoids showed the dysregulated expression of several signaling factors by which intestinal epithelium may modulate sensory neuron excitability, including proteases, cytokines, neuromodulators, growth factors, and hormones. These findings provide novel insights into the role of gut epithelium in the modulation of sensory neuron excitability under dysbiosis conditions, emphasizing that targeting epithelial-neuronal signaling might represent a promising therapeutic strategy for visceral pain management.

Original language	English
Article number	2547029
Journal	Gut Microbes
Volume	17
Issue number	1
DOIs	https://doi.org/10.1080/19490976.2025.2547029
Publication status	Published - 3 Sept 2025

Keywords

Visceral pain
organoids
epithelial-neuronal signaling
microbiota
dysbiosis
DRG neurons
intestinal epithelium

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This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1080/19490976.2025.2547029Licence: CC BY

Gut microbiota dysbiosis affects intestinal sensitivityFinal published version, 3.05 MBLicence: CC BY

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Margiotta, F., Lucarini, E., Toti, A., Curti, L., Masi, A., Mello, T., Le Gall, G., Mattei, G., Magi, A., Vauzour, D., Mannaioni, G., Di Cesare Mannelli, L., & Ghelardini, C. (2025). Gut microbiota dysbiosis affects intestinal sensitivity through epithelium-to-neuron signaling: novel insights from a colon organoid-based model to improve visceral pain therapy. Gut Microbes, 17(1), Article 2547029. https://doi.org/10.1080/19490976.2025.2547029

@article{13e01e6859024dce91f0a8eaad16dcdf,

title = "Gut microbiota dysbiosis affects intestinal sensitivity through epithelium-to-neuron signaling: novel insights from a colon organoid-based model to improve visceral pain therapy",

abstract = "Chronic gastrointestinal pain is a hallmark of most intestinal pathologies, yet effective treatments remain elusive given the complexity of the underlying mechanisms. Aiming to investigate the intestinal epithelium contribution to visceral pain modulation in dysbiosis context, we first demonstrated that intracolonic instillation of microbe-free fecal supernatants from mice with post-inflammatory dysbiosis induced by dextran sodium sulfate (FSDSS) provokes visceral hypersensitivity in recipient mice. Epithelium involvement in the response to FSDSS was analyzed through a novel in vitro approach comprising murine epithelial colon organoids and primary dorsal root ganglia (DRG) neurons. FSDSS treatment induced growth and metabolic impairment in colon organoids, which revealed a dysbiosis-driven epithelial dysfunction. Notably, the combination of FSDSS and conditioned medium from FSDSS-treated colon organoids induced an increase in DRG neuron intrinsic excitability, along with greater immunoreactivity to c-Fos and calcitonin-gene related peptide, implicating an integrated role of both microbial and epithelial products in visceral sensitivity regulation. By investigating the underlying signaling, metabolomic analysis revealed reduced levels of short chain fatty acids in FSDSS, such as butyrate, acetate, valerate, and propionate. Moreover, transcriptomic analysis of FSDSS-treated colon organoids showed the dysregulated expression of several signaling factors by which intestinal epithelium may modulate sensory neuron excitability, including proteases, cytokines, neuromodulators, growth factors, and hormones. These findings provide novel insights into the role of gut epithelium in the modulation of sensory neuron excitability under dysbiosis conditions, emphasizing that targeting epithelial-neuronal signaling might represent a promising therapeutic strategy for visceral pain management.",

keywords = "Visceral pain, organoids, epithelial-neuronal signaling, microbiota, dysbiosis, DRG neurons, intestinal epithelium",

author = "Francesco Margiotta and Elena Lucarini and Alessandra Toti and Lorenzo Curti and Alessio Masi and Tommaso Mello and {Le Gall}, Gwenaelle and Gianluca Mattei and Alberto Magi and David Vauzour and Guido Mannaioni and {Di Cesare Mannelli}, Lorenzo and Carla Ghelardini",

note = "Data availability statement: The RNA-seq data, including both raw FASTQ files and the resulting raw count matrices generated using Salmon, have been deposited in the NCBI Gene Expression Omnibus (GEO) database under accession number GSE294757. The other data that support the findings of this study are openly available in Mendeley Data at https://doi.org/10.17632/4k5yfp4nxd.1. Funding: This research was supported by the European Union - NextGenerationEU - National Recovery and Resilience Plan, Mission 4 Component 2 - Investment 1.5 - THE - Tuscany Health Ecosystem - ECS00000017 - CUP B83C22003920001; European Union - NextGenerationEU - National Recovery and Resilience Plan, Mission 4 Component 2 - Investment 1.4 – Strengthening research facilities and creation of “Campioni Nazionali di R&S” on Key Enabling Technologies - National Center for Gene Therapy and Drugs based on RNA Technology - CN00000041 - CUP B13C22001010001; and Italian Ministry of University and Research (MIUR) – “Dipartimenti di Eccellenza 2023-2027” - 58514_DIPECC_23_27- to the Department NEUROFARBA.",

year = "2025",

month = sep,

day = "3",

doi = "10.1080/19490976.2025.2547029",

language = "English",

volume = "17",

journal = "Gut Microbes",

issn = "1949-0976",

publisher = "Landes Bioscience",

number = "1",

}

Margiotta, F, Lucarini, E, Toti, A, Curti, L, Masi, A, Mello, T, Le Gall, G, Mattei, G, Magi, A, Vauzour, D, Mannaioni, G, Di Cesare Mannelli, L & Ghelardini, C 2025, 'Gut microbiota dysbiosis affects intestinal sensitivity through epithelium-to-neuron signaling: novel insights from a colon organoid-based model to improve visceral pain therapy', Gut Microbes, vol. 17, no. 1, 2547029. https://doi.org/10.1080/19490976.2025.2547029

TY - JOUR

T1 - Gut microbiota dysbiosis affects intestinal sensitivity through epithelium-to-neuron signaling: novel insights from a colon organoid-based model to improve visceral pain therapy

AU - Margiotta, Francesco

AU - Lucarini, Elena

AU - Toti, Alessandra

AU - Curti, Lorenzo

AU - Masi, Alessio

AU - Mello, Tommaso

AU - Le Gall, Gwenaelle

AU - Mattei, Gianluca

AU - Magi, Alberto

AU - Vauzour, David

AU - Mannaioni, Guido

AU - Di Cesare Mannelli, Lorenzo

AU - Ghelardini, Carla

N1 - Data availability statement: The RNA-seq data, including both raw FASTQ files and the resulting raw count matrices generated using Salmon, have been deposited in the NCBI Gene Expression Omnibus (GEO) database under accession number GSE294757. The other data that support the findings of this study are openly available in Mendeley Data at https://doi.org/10.17632/4k5yfp4nxd.1. Funding: This research was supported by the European Union - NextGenerationEU - National Recovery and Resilience Plan, Mission 4 Component 2 - Investment 1.5 - THE - Tuscany Health Ecosystem - ECS00000017 - CUP B83C22003920001; European Union - NextGenerationEU - National Recovery and Resilience Plan, Mission 4 Component 2 - Investment 1.4 – Strengthening research facilities and creation of “Campioni Nazionali di R&S” on Key Enabling Technologies - National Center for Gene Therapy and Drugs based on RNA Technology - CN00000041 - CUP B13C22001010001; and Italian Ministry of University and Research (MIUR) – “Dipartimenti di Eccellenza 2023-2027” - 58514_DIPECC_23_27- to the Department NEUROFARBA.

PY - 2025/9/3

Y1 - 2025/9/3

N2 - Chronic gastrointestinal pain is a hallmark of most intestinal pathologies, yet effective treatments remain elusive given the complexity of the underlying mechanisms. Aiming to investigate the intestinal epithelium contribution to visceral pain modulation in dysbiosis context, we first demonstrated that intracolonic instillation of microbe-free fecal supernatants from mice with post-inflammatory dysbiosis induced by dextran sodium sulfate (FSDSS) provokes visceral hypersensitivity in recipient mice. Epithelium involvement in the response to FSDSS was analyzed through a novel in vitro approach comprising murine epithelial colon organoids and primary dorsal root ganglia (DRG) neurons. FSDSS treatment induced growth and metabolic impairment in colon organoids, which revealed a dysbiosis-driven epithelial dysfunction. Notably, the combination of FSDSS and conditioned medium from FSDSS-treated colon organoids induced an increase in DRG neuron intrinsic excitability, along with greater immunoreactivity to c-Fos and calcitonin-gene related peptide, implicating an integrated role of both microbial and epithelial products in visceral sensitivity regulation. By investigating the underlying signaling, metabolomic analysis revealed reduced levels of short chain fatty acids in FSDSS, such as butyrate, acetate, valerate, and propionate. Moreover, transcriptomic analysis of FSDSS-treated colon organoids showed the dysregulated expression of several signaling factors by which intestinal epithelium may modulate sensory neuron excitability, including proteases, cytokines, neuromodulators, growth factors, and hormones. These findings provide novel insights into the role of gut epithelium in the modulation of sensory neuron excitability under dysbiosis conditions, emphasizing that targeting epithelial-neuronal signaling might represent a promising therapeutic strategy for visceral pain management.

AB - Chronic gastrointestinal pain is a hallmark of most intestinal pathologies, yet effective treatments remain elusive given the complexity of the underlying mechanisms. Aiming to investigate the intestinal epithelium contribution to visceral pain modulation in dysbiosis context, we first demonstrated that intracolonic instillation of microbe-free fecal supernatants from mice with post-inflammatory dysbiosis induced by dextran sodium sulfate (FSDSS) provokes visceral hypersensitivity in recipient mice. Epithelium involvement in the response to FSDSS was analyzed through a novel in vitro approach comprising murine epithelial colon organoids and primary dorsal root ganglia (DRG) neurons. FSDSS treatment induced growth and metabolic impairment in colon organoids, which revealed a dysbiosis-driven epithelial dysfunction. Notably, the combination of FSDSS and conditioned medium from FSDSS-treated colon organoids induced an increase in DRG neuron intrinsic excitability, along with greater immunoreactivity to c-Fos and calcitonin-gene related peptide, implicating an integrated role of both microbial and epithelial products in visceral sensitivity regulation. By investigating the underlying signaling, metabolomic analysis revealed reduced levels of short chain fatty acids in FSDSS, such as butyrate, acetate, valerate, and propionate. Moreover, transcriptomic analysis of FSDSS-treated colon organoids showed the dysregulated expression of several signaling factors by which intestinal epithelium may modulate sensory neuron excitability, including proteases, cytokines, neuromodulators, growth factors, and hormones. These findings provide novel insights into the role of gut epithelium in the modulation of sensory neuron excitability under dysbiosis conditions, emphasizing that targeting epithelial-neuronal signaling might represent a promising therapeutic strategy for visceral pain management.

KW - Visceral pain

KW - organoids

KW - epithelial-neuronal signaling

KW - microbiota

KW - dysbiosis

KW - DRG neurons

KW - intestinal epithelium

U2 - 10.1080/19490976.2025.2547029

DO - 10.1080/19490976.2025.2547029

M3 - Article

SN - 1949-0976

VL - 17

JO - Gut Microbes

JF - Gut Microbes

IS - 1

M1 - 2547029

ER -