Gliadin-dependent neuromuscular and epithelial secretory responses in gluten-sensitive HLA-DQ8 transgenic mice

doi:10.1152/ajpgi.00225.2007

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Am J Physiol Gastrointest Liver Physiol 294: G217-G225, 2008. First published November 15, 2007; doi:10.1152/ajpgi.00225.2007
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NEUROREGULATION AND MOTILITY

Gliadin-dependent neuromuscular and epithelial secretory responses in gluten-sensitive HLA-DQ8 transgenic mice

E. F. Verdu,¹ X. Huang,¹ J. Natividad,¹ J. Lu,¹ P. A. Blennerhassett,¹ C. S. David,² D. M. McKay,¹ and J. A. Murray³

¹Intestinal Disease Research Program, McMaster University, Hamilton, Ontario, Canada; and ²Department of Immunology, and ³Division of Gastroenterology, Mayo Clinic, Rochester, Minnesota

Submitted 18 May 2007 ; accepted in final form 6 November 2007

Celiac disease is a gluten intolerance caused by a T-cell responseagainst human leukocyte antigen (HLA)-DQ2 and DQ8-bound glutenpeptides. Some subjects experience gastrointestinal symptomsin the absence of villous atrophy. Here we investigate the potentialmechanisms of gut dysfunction in gluten-sensitive HLA-DQ8 transgenicmice. HLA-DQ8 mice were sensitized and gavaged with gliadin3x/wk for 3 wk (G/G). Controls included 1) nonsensitized micegavaged with rice (C); 2) gliadin-sensitized mice gavaged withrice (G/R); and 3) BSA-sensitized mice gavaged with BSA (BSA/BSA).CD3⁺ intraepithelial lymphocyte, macrophage, and FOX-P3-positivecell counts were determined. Acetylcholine release, small intestinalcontractility, and epithelial ion transport were measured. Gutfunction was investigated after gluten withdrawal and in HLA-DQ6mice. Intestinal atrophy was not observed in G/G mice. Recruitmentof intraepithelial lymphocyte, macrophages, and FOX-P3+ cellswere observed in G/G, but not in C, G/R, or BSA/BSA mice. Thiswas paralleled by increased acetylcholine release from the myentericplexus, muscle hypercontractility, and increased active iontransport in G/G mice. Changes in muscle contractility normalizedin DQ8 mice after a gluten withdrawal. HLA-DQ6 controls didnot exhibit the abnormalities in gut function observed in DQ8mice. Gluten sensitivity in HLA-DQ8 mice induces immune activationin the absence of intestinal atrophy. This is associated withcholinergic dysfunction and a prosecretory state that may leadto altered water movements and dysmotility. The results providea mechanism by which gluten could induce gut dysfunction inpatients with a genetic predisposition but without fully evolvedceliac disease.

muscle contractility; intestinal ion transport; food sensitivity

Address for reprint requests and other correspondence: E. F. Verdu, 1200 Main W, McMaster Univ., HSC 3N5C, Hamilton, Ontario, Canada (e-mail: verdue{at}mcmaster.ca)