Traces of Canine Inflammatory Bowel Disease Reflected by Intestinal Organoids

Int J Mol Sci. 2024 Jan 1;25(1):576. doi: 10.3390/ijms25010576.

Abstract

Inflammatory bowel disease (IBD) is a chronic inflammatory condition that affects humans and several domestic animal species, including cats and dogs. In this study, we have analyzed duodenal organoids derived from canine IBD patients using quantitative proteomics. Our objective was to investigate whether these organoids show phenotypic traits of the disease compared with control organoids obtained from healthy donors. To this aim, IBD and control organoids were subjected to quantitative proteomics analysis via liquid chromatography-mass spectrometry. The obtained data revealed notable differences between the two groups. The IBD organoids exhibited several alterations at the levels of multiple proteins that are consistent with some known IBD alterations. The observed phenotype in the IBD organoids to some degree mirrors the corresponding intestinal condition, rendering them a compelling approach for investigating the disease and advancing drug exploration. Additionally, our study revealed similarities to some human IBD biomarkers, further emphasizing the translational and comparative value of dogs for future investigations related to the causes and treatment of IBD. Relevant proteins such as CALU, FLNA, MSN and HMGA2, which are related to intestinal diseases, were all upregulated in the IBD duodenal organoids. At the same time, other proteins such as intestinal keratins and the mucosal immunity PIGR were depleted in these IBD organoids. Based on these findings, we propose that these organoids could serve as a valuable tool for evaluating the efficacy of therapeutic interventions against canine IBD.

Keywords: IBD; canine IBD; chronic enteropathy; disease modeling; inflammatory bowel diseases; organoid.

MeSH terms

  • Animals
  • Animals, Domestic
  • Cats
  • Dogs
  • Duodenum
  • Humans
  • Inflammatory Bowel Diseases* / veterinary
  • Intestines*
  • Organoids

Grants and funding

This research was funded by The Austrian Research Association FFG, project number 13610974. G.C. was funded by the Austrian Academy of Sciences (ÖAW) DOC fellowship, grant number 26349. Open Access Funding by the University of Veterinary Medicine Vienna.