A Screening Approach for Identifying Gliadin Neutralizing Antibodies on Epithelial Intestinal Caco-2 Cells

Harald Hundsberger(IMC University of Applied Sciences Krems), Anita Koppensteiner(IMC University of Applied Sciences Krems), Elisabeth Hofmann(IMC University of Applied Sciences Krems), Doris Ripper(IMC University of Applied Sciences Krems), Maren Pflüger(IMC University of Applied Sciences Krems), Valerie Stadlmann(Universitätsklinikum Tulln), Christian Klein(IMC University of Applied Sciences Krems), Birgit Kreiseder(IMC University of Applied Sciences Krems), Michael Katzlinger(Molecular Devices (United Kingdom)), Andreas Eger(IMC University of Applied Sciences Krems), Florian Forster(Universitätsklinikum Tulln), Albert Mißbichler(Universitätsklinikum Tulln), Christoph Wiesner(IMC University of Applied Sciences Krems)
SLAS DISCOVERY
May 26, 2017
Cited by 8Open Access
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Abstract

Celiac disease (CD) is a chronic inflammatory condition caused by the ingestion of gliadin-containing food in genetically susceptible individuals. Undigested peptides of gliadin exert various effects, including increased intestinal permeability and inflammation in the small intestine. Although many therapeutic approaches are in development, a gluten-free diet is the only effective treatment for CD. Affecting at least 1% of the population in industrialized countries, it is important to generate therapeutic options against CD. Here, we describe the establishment of a high-throughput screening (HTS) platform based on AlphaLISA and electrical cell-substrate impedance sensing (ECIS) technology for the identification of anti-inflammatory and barrier-protective compounds in human enterocytes after pepsin-trypsin-digested gliadin (PT-gliadin) treatment. Our results show that the combination of these HTS technologies enables fast, reliable, simple, and label-free screening of IgY antibodies against PT-gliadin. Using this platform, we have identified a new chicken anti-PT-gliadin IgY antibody as a potential anti-CD agent.


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