# Uncovering the therapeutic potential of anti-tuberculoid agent Isoniazid in a model of microbial-driven Crohn’s disease

**Authors:** Matthew Stephens, Keith Keane, Simon Roizes, Manon Defaye, Christophe Altier, Pierre-Yves von der Weid

PMC · DOI: 10.1093/ecco-jcc/jjaf032 · Journal of Crohn's & Colitis · 2025-02-23

## TL;DR

This study shows that Isoniazid, a TB drug, can reduce intestinal inflammation in a mouse model of Crohn’s disease by limiting harmful bacteria.

## Contribution

Isoniazid's TB-independent therapeutic potential in Crohn’s disease is revealed through its effect on pathobiont bacteria and inflammation.

## Key findings

- Isoniazid reduces both intestinal and systemic inflammation in TNFΔARE mice.
- Isoniazid limits the expansion of segmented filamentous bacteria (SFB) in the gut.
- Reduced SFB is linked to fewer precursor-tertiary lymphoid organs in the ileal mesentery.

## Abstract

TNFα has long stood as a hallmark feature of both inflammatory bowel disease and arthritis with its therapeutic potential demonstrated in neutralizing monoclonal antibody treatments such as Infliximab. Due to the high global burden of latent Mycobacterium tuberculosis (TB) infections, prior to receiving anti-TNF therapy, patients testing positive for latent TB are given prophylactic treatment with anti-tuberculoid medications including the first described TB-selective antibiotic, Isoniazid. While this is common clinical practice to prevent the emergence of TB, little is known about whether Isoniazid modifies intestinal inflammation alone. The aim of this study, therefore, was to determine whether Isoniazid presents a novel TB-independent therapeutic option for the treatment of Crohn’s disease (CD)-like ileitis and uncover new mechanisms predisposing the host to intestinal inflammation.

The transgenic TNFΔARE mouse model of Crohn’s-like terminal ileitis was used. The impact of Isoniazid administration (10 mg/kg/day dose in drinking water) on disease development was monitored between 8 and 12 weeks of age using a variety of behavioral and serological assays. Behavioral and motor functions were assessed using the LABORAS automated monitoring system while systemic and local tissue inflammation were determined at experimental termination using multiplex cytokine analysis. Whole-mount tissue immunofluorescence and fluorescent in situ hybridization were used to qualify changes within the host as well as the microbial compartment of the ileum and associated mesentery. Proposed cellular mechanisms of altered cytokine decay were performed on isolated primary splenocytes in vitro using selective pharmacological agents.

Compared to age-matched wild-type littermates, TNFΔARE mice display prominent progressive sickness behaviors from 8 through 12 weeks of age indicated by reduced movement, climbing, and rearing. Prophylactic administration of Isoniazid (10 mg/kg/day) is effectively able to protect TNFΔARE mice from this loss of function during the same period. Analysis revealed that Isoniazid was able to significantly reduce both systemic and intestinal inflammation compared to untreated vehicle controls impacting the epithelial colonization of known pathobiont segmented filamentous bacteria (SFB). Reduction in terminal ileal inflammation was also associated to the diminished formation of precursor-tertiary lymphoid organs within the associated ileal mesentery which were found to be associated with endospores derived SFB itself. Finally, we reveal that due to their genetic manipulation, TNFΔARE mice display accelerated posttranscriptional decay of IL-22 mRNA resulting in diminished IL-22 protein production and associated downstream antimicrobial peptide production.

Isoniazid protects against the development of intestinal and systemic inflammation in the TNFΔARE model of terminal ileitis by limiting the expansion of mucosal SFB and progression of the associated microbial-driven inflammation. This work highlights a possible mycobacterial-independent function of Isoniazid in limiting CD pathophysiology through limiting the mucosal establishment of pathobionts such as SFB and the association of such microbe-derived endospores linked to the formation of ectopic tertiary lymphoid organs seen commonly in patients.

Graphical Abstract

## Linked entities

- **Proteins:** TNF (tumor necrosis factor), IL22 (interleukin 22)
- **Chemicals:** Isoniazid (PubChem CID 3767)
- **Diseases:** Crohn’s disease (MONDO:0005011), arthritis (MONDO:0005578), inflammatory bowel disease (MONDO:0005265), tuberculosis (MONDO:0018076)
- **Species:** Mus musculus (taxon 10090)

## Full-text entities

- **Genes:** TNF (tumor necrosis factor) [NCBI Gene 7124] {aka DIF, IMD127, TNF-alpha, TNFA, TNFSF2, TNLG1F}
- **Diseases:** IBD (MESH:D015212), arthritis (MESH:D001168), Mycobacterium tuberculosis (TB) infections (MESH:D014376), inflammation (MESH:D007249), ileitis (MESH:D007079), CD (MESH:D003424)
- **Chemicals:** Isoniazid (MESH:D007538), Infliximab (MESH:D000069285)
- **Species:** Homo sapiens (human, species) [taxon 9606], Mus musculus (house mouse, species) [taxon 10090]

## Full text

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## Figures

8 figures with captions in the complete paper: https://tomesphere.com/paper/PMC11920797/full.md

## References

85 references — full list in the complete paper: https://tomesphere.com/paper/PMC11920797/full.md

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Source: https://tomesphere.com/paper/PMC11920797