A Quantitative Analysis of Transglutaminase 2-Mediated Deamidation of Gluten Peptides: Implications for the T-cell Response in Celiac Disease

Dørum, Siri; Qiao, Shuo‐Wang; Sollid, Ludvig M.; Fleckenstein, Burkhard

doi:10.1021/pr800960n

Cited by 40 publications

(34 citation statements)

References 92 publications

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“…Variant peptides that displayed a serine (S) at position 5 instead of an phenylalaninine (F) were found to have lost T-cell stimulatory capacity. Moreover, the presence of a positively charged arginine (R) residue at position +1 diminished T-cell proliferation (Additional file 3), most likely because it influenced the deamidation of Q9 as previously observed by Dørum et al [28]. Similarly, a tryptophan (W) at position +2 inhibited the T-cell response (Additional file 3).…”

Section: Discussionsupporting

confidence: 57%

Celiac disease T-cell epitopes from gamma-gliadins: immunoreactivity depends on the genome of origin, transcript frequency, and flanking protein variation

Salentijn¹,

Mitea

Goryunova

et al. 2012

BMC Genomics

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BackgroundCeliac disease (CD) is caused by an uncontrolled immune response to gluten, a heterogeneous mixture of wheat storage proteins. The CD-toxicity of these proteins and their derived peptides is depending on the presence of specific T-cell epitopes (9-mer peptides; CD epitopes) that mediate the stimulation of HLA-DQ2/8 restricted T-cells. Next to the thoroughly characterized major T-cell epitopes derived from the α-gliadin fraction of gluten, γ-gliadin peptides are also known to stimulate T-cells of celiac disease patients. To pinpoint CD-toxic γ-gliadins in hexaploid bread wheat, we examined the variation of T-cell epitopes involved in CD in γ-gliadin transcripts of developing bread wheat grains.ResultsA detailed analysis of the genetic variation present in γ-gliadin transcripts of bread wheat (T. aestivum, allo-hexaploid, carrying the A, B and D genome), together with genomic γ-gliadin sequences from ancestrally related diploid wheat species, enabled the assignment of sequence variants to one of the three genomic γ-gliadin loci, Gli-A1, Gli-B1 or Gli-D1. Almost half of the γ-gliadin transcripts of bread wheat (49%) was assigned to locus Gli-D1. Transcripts from each locus differed in CD epitope content and composition. The Gli-D1 transcripts contained the highest frequency of canonical CD epitope cores (on average 10.1 per transcript) followed by the Gli-A1 transcripts (8.6) and the Gli-B1 transcripts (5.4). The natural variants of the major CD epitope from γ-gliadins, DQ2-γ-I, showed variation in their capacity to induce in vitro proliferation of a DQ2-γ-I specific and HLA-DQ2 restricted T-cell clone.ConclusionsEvaluating the CD epitopes derived from γ-gliadins in their natural context of flanking protein variation, genome specificity and transcript frequency is a significant step towards accurate quantification of the CD toxicity of bread wheat. This approach can be used to predict relative levels of CD toxicity of individual wheat cultivars directly from their transcripts (cDNAs).

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Section: Discussionsupporting

confidence: 57%

Celiac disease T-cell epitopes from gamma-gliadins: immunoreactivity depends on the genome of origin, transcript frequency, and flanking protein variation

Salentijn¹,

Mitea

Goryunova

et al. 2012

BMC Genomics

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“…TGase-mediated glutamine deamidation is a well known PTM found in dietary gluten protein, which in turn results in an increased T-cell response (44). The high glutamine substrate affinity for TGase cross-linking found in Tau protein is of particular interest here (45), because glutamine deamidation may trigger misfolding of Tau (46), ␣-synuclein, and Huntington protein.…”

Section: Discussionmentioning

confidence: 99%

Tissue Transglutaminase-mediated Glutamine Deamidation of β-Amyloid Peptide Increases Peptide Solubility, Whereas Enzymatic Cross-linking and Peptide Fragmentation May Serve as Molecular Triggers for Rapid Peptide Aggregation

Schmid

Condemi

Tuchscherer

et al. 2011

Journal of Biological Chemistry

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Tissue transglutaminase (TGase) has been implicated in a number of cellular processes and disease states, where the enzymatic actions of TGase may serve in both, cell survival and apoptosis. To date, the precise functional properties of TGase in cell survival or cell death mechanisms still remain elusive. TGasemediated cross-linking has been reported to account for the formation of insoluble lesions in conformational diseases. We report here that TGase induces intramolecular cross-linking of ␤-amyloid peptide (A␤), resulting in structural changes of monomeric A␤. Using high resolution mass spectrometry (MS) of cross-linked A␤ peptides, we observed a shift in mass, which is, presumably associated with the loss of NH 3 due to enzymatic transamidation activity and hence intramolecular peptide cross-linking. We have observed that a large population of A␤ monomers contained an 0.984 Da increase in mass at a glutamine residue, indicating that glutamine 15 serves as an indispensable substrate in TGase-mediated deamidation to glutamate 15. We provide strong analytical evidence on TGasemediated A␤ peptide dimerization, through covalent intermolecular cross-linking and hence the formation of A␤ 1-40 dimers. Our in depth analyses indicate that TGase-induced post-translational modifications of A␤ peptide may serve as an important seed for aggregation.

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“…Only glutamine residues residing in the sequence QXP, where Q is glutamine, X is any amino acid and P is proline, are targeted by the enzyme [35,36], providing yet an explanation for the high proline content in gluten T-cell epitopes. Interestingly, it was found that those peptides that are most efficiently deamidated are also the ones that are most frequently recognized by T cells in celiac disease patients [37], pointing at a central role for TG2 in shaping the anti-gluten T-cell repertoire. This was signified by the finding that within a complex mixture of gluten peptides, TG2 selectively targeted peptides harboring known T-cell epitopes [38].…”

Section: Substrate Affinity To Transglutaminase-2 (Tg2)mentioning

confidence: 99%

T-cell and B-cell immunity in celiac disease

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Sollid

2015

Best Practice & Research Clinical Gastroenterology

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A Quantitative Analysis of Transglutaminase 2-Mediated Deamidation of Gluten Peptides: Implications for the T-cell Response in Celiac Disease

Cited by 40 publications

References 92 publications

Celiac disease T-cell epitopes from gamma-gliadins: immunoreactivity depends on the genome of origin, transcript frequency, and flanking protein variation

Celiac disease T-cell epitopes from gamma-gliadins: immunoreactivity depends on the genome of origin, transcript frequency, and flanking protein variation

Tissue Transglutaminase-mediated Glutamine Deamidation of β-Amyloid Peptide Increases Peptide Solubility, Whereas Enzymatic Cross-linking and Peptide Fragmentation May Serve as Molecular Triggers for Rapid Peptide Aggregation

T-cell and B-cell immunity in celiac disease

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