Abstract
Crohn’s Disease (CD) is incurable, and represents a lifelong burden for patients and its incidence is increasing worldwide. A key contributing factor is a dysregulated immune response. Here we report the generation of genome edited pigs with a deletion of the transcript-destabilizing AU-rich element (ARE) and a constitutive decay element (CDE) in the TNF gene which recapitulate major characteristics of human CD, including ulcerative transmural ileocolitis, increased abundance of proinflammatory cytokines, evidence for impaired integrity of the intestinal epithelial cell barrier, immune cell infiltration, and dysbiotic microbial communities. This physiologically relevant CD model enables human-scale and long-term studies to assess diagnostic, nutritional or microbial interventions, filling the gap for translating findings into the clinic.
Competing Interest Statement
The authors have declared no competing interest.
Footnotes
Grant support: This work was supported by Deutsche Forschungsgemeinschaft (DFG, German Research Foundation) – Projektnummer 395357507 – SFB 1371.
Disclosures: The authors declare no conflicts of interest.
Writing assistance: None.
DNA sequence data: NCBI accession number GCF_000003025.6, Sscrofa 11.1
Abbreviations used in this paper
- IBD
- Inflammatory bowel disease
- CD
- Crohn’s disease
- TNF
- Tumor necrosis factor alpha
- ARE
- AU-rich element
- CDE
- Constitutive decay element
- Ki67
- Marker of proliferation Ki67 (Kiel-67)
- CD3
- Cluster of differentiation 3
- IBA1
- Allograft inflammatory factor 1
- IL6
- Interleukin-6
- IL8
- Interleukin-8
