AI Article Synopsis

  • Advances in mass spectrometry and bioinformatics now allow for global analysis of tissue proteomes from small biopsy samples, particularly useful in studying celiac disease (CD).
  • In CD, gluten triggers an immune response that alters the small intestine; removing gluten normalizes tissue structure and immune activity.
  • This study compared protein expression in biopsy samples before and after a gluten-free diet or after gluten provocation, identifying specific proteins that distinguish treated from untreated CD and revealing markers like IGHV5-51 for ongoing immune activation.

Article Abstract

Global characterization of tissue proteomes from small amounts of biopsy material has become feasible because of advances in mass spectrometry and bioinformatics tools. In celiac disease (CD), dietary gluten induces an immune response that is accompanied by pronounced remodeling of the small intestine. Removal of gluten from the diet abrogates the immune response, and the tissue architecture normalizes. In this study, differences in global protein expression of small intestinal biopsy specimens from CD patients were quantified by analyzing formalin-fixed, paraffin-embedded material using liquid chromatography-mass spectrometry and label-free protein quantitation. Protein expression was compared in biopsy specimens collected from the same patients before and after 1-year treatment with gluten-free diet (n = 10) or before and after 3-day gluten provocation (n = 4). Differential expression of proteins in particular from mature enterocytes, neutrophils, and plasma cells could distinguish untreated from treated CD mucosa, and Ig variable region IGHV5-51 expression was found to serve as a CD-specific marker of ongoing immune activation. In patients who had undergone gluten challenge, coordinated up-regulation of wound response proteins, including the CD autoantigen transglutaminase 2, was observed. Our study provides a global and unbiased assessment of antigen-driven changes in protein expression in the celiac intestinal mucosa.

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Source
http://dx.doi.org/10.1016/j.ajpath.2018.03.017DOI Listing

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