| Literature DB >> 28345372 |
Svenja Ley1, Olaf Galuba1, Adrian Salathe1, Nicolas Melin1, Alexandra Aebi1, Monika Pikiolek1, Judith Knehr1, Walter Carbone1, Martin Beibel1, Florian Nigsch1, Guglielmo Roma1, Giovanni d'Ario1, Susan Kirkland1, Laure C Bouchez1, Caroline Gubser Keller1, Tewis Bouwmeester1, Christian N Parker1, Heinz Ruffner1.
Abstract
Oral and intestinal mucositis is a debilitating side effect of radiation treatment. A mouse model of radiation-induced mucositis leads to weight loss and tissue damage, reflecting the human ailment as it responds to keratinocyte growth factor (KGF), the standard-of-care treatment. Cultured intestinal crypt organoids allowed the development of an assay monitoring the effect of treatments of intestinal epithelium to radiation-induced damage. This in vitro assay resembles the mouse model as KGF and roof plate-specific spondin-1 (RSPO1) enhanced crypt organoid recovery following radiation. Screening identified compounds that increased the survival of organoids postradiation. Testing of these compounds revealed that the organoids changed their responses over time. Unbiased transcriptome analysis was performed on crypt organoid cultures at various time points in culture to investigate this adaptive behavior. A number of genes and pathways were found to be modulated over time, providing a rationale for the altered sensitivity of the organoid cultures. This report describes an in vitro assay that reflects aspects of human disease. The assay was used to identify bioactive compounds, which served as probes to interrogate the biology of crypt organoids over prolonged culture. The pathways that are changing over time may offer potential targets for treatment of mucositis.Entities:
Keywords: KGF; RSPO; mucositis; primary 3D cell cultures; small intestinal crypt organoids
Mesh:
Substances:
Year: 2017 PMID: 28345372 DOI: 10.1177/2472555216683651
Source DB: PubMed Journal: SLAS Discov ISSN: 2472-5552 Impact factor: 3.341