4.7 Article

Experimental hookworm infection and gluten microchallenge promote tolerance in celiac disease

Journal

JOURNAL OF ALLERGY AND CLINICAL IMMUNOLOGY
Volume 135, Issue 2, Pages 508-U677

Publisher

MOSBY-ELSEVIER
DOI: 10.1016/j.jaci.2014.07.022

Keywords

Celiac disease; gluten; hookworm; autoimmunity; helminth therapy; desensitization; mucosal immunology; regulatory T cells; intra-epithelial lymphocytes

Funding

  1. Australian National Health and Medical Research Council (NHMRC) Program Grant [1037304]
  2. NHMRC Overseas Biomedical Fellowship [613718]
  3. NHMRC Principal Research Fellowship [1020114]
  4. NHMRC Senior Research Fellowship [1058685]
  5. NHMRC Practitioner Fellowship
  6. Government of Queensland Health Research Fellowship [1041802]
  7. Far North Queensland Hospital Foundation Small Research Grant
  8. National Health and Medical Research Council of Australia [1058685] Funding Source: NHMRC

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Background: Celiac disease (CeD) is a common gluten-sensitive autoimmune enteropathy. A gluten-free diet is an effective treatment, but compliance is demanding; hence, new treatment strategies for CeD are required. Objective: Parasitic helminths hold promise for treating inflammatory disorders, so we examined the influence of experimental hookworm infection on the predicted outcomes of escalating gluten challenges in CeD subjects. Methods: A 52-week study was conducted involving 12 adults with diet-managed CeD. Subjects were inoculated with 20 Necator americanus larvae, and escalating gluten challenges consumed as pasta were subsequently administered: (1) 10 to 50 mg for 12 weeks (microchallenge); (2) 25 mg daily + 1 g twice weekly for 12 weeks (GC-1g); and (3) 3 g daily (60-75 straws of spaghetti) for 2 weeks (GC-3g). Symptomatic, serologic, and histological outcomes evaluated gluten toxicity. Regulatory and inflammatory T cell populations in blood and mucosa were examined. Results: Two gluten-intolerant subjects were withdrawn after microchallenge. Ten completed GC-1g, 8 of whom enrolled in and completed GC-3g. Primary outcomes: median villous height-to-crypt depth ratios (2.60-2.63; P = .98) did not decrease as predicted after GC-1g, and the mean IgA-tissue transglutaminase titers declined, contrary to the predicted rise after GC-3g. Secondary outcomes: quality of life scores improved (46.3-40.6; P = .05); celiac symptom indices (24.3-24.3; P = .53), intra-epithelial lymphocyte percentages (32.5-35.0; P = .47), and Marsh scores were unchanged by gluten challenge. Intestinal T cells expressing IFN gamma were reduced following hookworm infection (23.9%-11.5%; P = .04), with corresponding increases in CD4(+) Foxp3(+) regulatory T cells (0.19%-1.12%; P = .001). Conclusions: Necator americanus and gluten microchallenge promoted tolerance and stabilized or improved all tested indices of gluten toxicity in CeD subjects.

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