3D organoids and organoid derived monolayers from patients with inflammatory bowel disease
Scope of the method
- Human health
- Basic Research
- Education and training
- Translational - Applied Research
- In vitro - Ex vivo
- Human derived cells / tissues / organs
Description
- organoids
- ECM
- 3D culture
- Coculture model
- Transwell
- inflammatory bowel disease
- ulcerative colitis
- crohn's disease
- stem cells
- epithelial cells
- intestinal crypt
Intestinal organoids are cultured from intestinal biopsies obtained during routine endoscopy. The stem cell containing crypts are isolated and cultured in a 3D ECM (Matrigel) in the presence of the desired growth factors. The present stem cells will expand and give rise to all epithelial cells of the intestinal epithelium while maintaining location, disease and patient specific characteristics. 3D organoids can be used to evaluate several mechanism including responses to inflammatory stimuli, microbiota stimulation, analysis of epithelial (transport) mechanisms in the development/progress of IBD. In addition, 3D organoids can be dissociated and seeded into 2D transwells to allow access to the apical side of the cells for exposure towards different components.
- - Biosafety cabinet ;
- - CO2 cell incubator ;
- - Centrifuge Microscope.
- Published in peer reviewed journal
Pros, cons & Future potential
Organoids and organoid derived monolayers maintain region, disease and patient-specific characteristics.
- - Only epithelial cells (no immune cells) present.
- - Requires specialized training ECM and medium including growth factors is rather expensive.
- - Organoids can be cultured from multiple organs.
- - Possibilities for co-culture with other cell-types are being explored.
Organoids have/are currently been/being developed from different organs and are widely applied for the analysis of different mechanisms (drug testing, barrier function, specific mutations,..).
References, associated documents and other information
Arnauts K, Verstockt B, Santo Ramalho Veñancio A, et al. Ex vivo mimicking of inflammation in organoids derived from patients with ulcerative colitis. Gastroenterology 2020, in press. https://doi.org/10.1053/j.gastro.2020.05.064
Vancamelbeke M, Laeremans T, Vanhove W, et al. Butyrate Does Not Protect Against Inflammation-induced Loss of Epithelial Barrier Function and Cytokine Production in Primary Cell Monolayers From Patients With Ulcerative Colitis. J Crohns Colitis. 2019;13(10):1351‐1361. doi:10.1093/ecco-jcc/jjz064
Noben M, Verstockt B, de Bruyn M, et al. Epithelial organoid cultures from patients with ulcerative colitis and Crohn's disease: a truly long-term model to study the molecular basis for inflammatory bowel disease?. Gut. 2017;66(12):2193‐2195. doi:10.1136/gutjnl-2016-313667
Noben M, Vanhove W, Arnauts K, et al. Human intestinal epithelium in a dish: Current models for research into gastrointestinal pathophysiology. United European Gastroenterol J. 2017;5(8):1073‐1081. doi:10.1177/2050640617722903
Contact person
Bram VerstocktOrganisations
Katholieke Universiteit Leuven (KUL)Department of Chronic Diseases and Metabolism
Translational Research in GastroIntestinal Disorders (TARGID) - IBD Group
Belgium
Flemish Region