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Maki, M. and Caporale, D. HLA-DQ1 Alpha and Beta Genotypes Associated with Non-Celiac Gluten Sensitivity. The FASEB Journal, 2018; 31(1).

has been cited by the following article:

Article

Relationship Between Genotype and Disease Phenotype for Gluten-Related Disorders

1Department of Biology, Linfield University, McMinnville, Oregon 97128 USA

2Celiac Nurse Consulting, Salem, Oregon 97302 USA

3Department of Mathematics and Computer Science, Linfield University, McMinnville, Oregon 97128 USA


International Journal of Celiac Disease. 2024, Vol. 12 No. 1, 33-40
DOI: 10.12691/ijcd-12-1-7
Copyright © 2024 Science and Education Publishing

Cite this paper:
Michael F. Roberts, Nadine Grzeskowiak, Stephen E. Bricher. Relationship Between Genotype and Disease Phenotype for Gluten-Related Disorders. International Journal of Celiac Disease. 2024; 12(1):33-40. doi: 10.12691/ijcd-12-1-7.

Correspondence to: Michael  F. Roberts, Department of Biology, Linfield University, McMinnville, Oregon 97128 USA. Email: mrobert@linfield.edu

Abstract

We investigated gluten-related disorders (GRD) in intestinal biopsy-proven subjects to determine the relation between genotype (i.e., Human Leukocyte Antigen (HLA) DQ alleles) and phenotype (i.e., antibody levels and clearly defined symptoms). Subjects had known DQ genotypes, information on IgA anti-Endomysial antibodies (EMA) and/or anti-tissue Trans Glutaminase (tTG) antibodies (tTGA). Subjects also answered a survey characterizing gastrointestinal, skin, and neural symptoms. Though all were biopsy-proven, HLA genotypes included all combinations of DQ2.5, DQ2.2, DQ8, DQ7.5, DQ5, and DQ6. Subject antibody levels were proportional to the number of DQ2.5 haplotypes, and subjects with non-CD-associated haplotypes did not have positive antibody scores (despite positive biopsy). In addition, the total number of GRD-associated symptoms were approximately the same across all genotypes. The results suggest that gluten damage and symptoms are independent of genotype; i.e., not restricted to people with DQ2.5, DQ2.2, or DQ8 genotypes or to those with positive antibody scores. We propose a GRD classification in which clinicians consider GRD symptoms and signs even in people without CD-associated genotypes, as these likely make up the majority of those with gluten-related disorders.

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