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Evaluation of Intestinal Epithelial Barrier Function in Inflammatory Bowel Diseases Using Murine Intestinal Organoids

Authors
Rallabandi, Harikrishna ReddyYang, HyeonOh, Keon BongLee, Hwi CheulByun, Sung JuneLee, Bo Ram
Issue Date
Oct-2020
Publisher
KOREAN TISSUE ENGINEERING REGENERATIVE MEDICINE SOC
Keywords
Intestinal stem cells; Organoids; IBD; Epithelial barrier; Ex vivomodel
Citation
TISSUE ENGINEERING AND REGENERATIVE MEDICINE, v.17, no.5, pp.641 - 650
Journal Title
TISSUE ENGINEERING AND REGENERATIVE MEDICINE
Volume
17
Number
5
Start Page
641
End Page
650
URI
https://scholarworks.bwise.kr/gachon/handle/2020.sw.gachon/81229
DOI
10.1007/s13770-020-00278-0
ISSN
1738-2696
Abstract
Background: Intestinal organoids have evolved as potential molecular tools that could be used to study host-microbiome interactions, nutrient uptake, and drug screening. Gut epithelial barrier functions play a crucial role in health and diseases, especially in autoimmune diseases, such as inflammatory bowel diseases (IBDs), because they disrupt the epithelial mucosa and impair barrier function. Methods: In this study, we generated anin vitroIBD model based on dextran sodium sulfate (DSS) and intestinal organoids that could potentially be used to assess barrier integrity. Intestinal organoids were long-term cultivated and characterized with several specific markers, and the key functionality of paracellular permeability was determined using FITC-dextran 4 kDa. Intestinal organoids that had been treated with 2 mu M DSS for 3 h were developed and the intestinal epithelial barrier function was sequentially evaluated. Results: The results indicated that the paracellular permeability represented epithelial characteristics and their barrier function had declined when they were exposed to FITC-dextran 4 kDa after DSS treatment. In addition, we analyzed the endogenous mRNA expression of pro-inflammatory cytokines and their downstream effector genes. The results demonstrated that the inflammatory cytokines genes significantly increased in inflamed organoids compared to the control, leading to epithelial barrier damage and dysfunction. Conclusion: The collective results showed thatin vitro3D organoids mimicin vivotissue topology and functionality with minor limitations, and hence are helpful for testing disease models.
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