Immune Cross-Reactivity in Celiac Disease: Anti-Gliadin Antibodies Bind to Neuronal Synapsin I

Alaedini, Armin; Okamoto, Haruka; Briani, Chiara; Wollenberg, Kurt; Shill, Holly A.; Bushara, Khalafalla O.; Sander, Howard W.; Green, Peter H.R.; Hallett, Mark; Latov, Norman

doi:10.4049/jimmunol.178.10.6590

Cited by 99 publications

(78 citation statements)

References 40 publications

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“…Collection of serum for immunoblotting and immunoflouorescence analyses was done on day 0 (preimmunization) and day 55 (postimmunization). Abs from pooled sera for each peptide immunization were purified by affinity chromatography, using peptidecoupled affinity columns, as described previously (32). Reactivity of the generated rabbit sera and affinity-purified Abs to each peptide was confirmed at serial dilutions by ELISA, using the same procedure as described above, except HRP-conjugated donkey anti-rabbit IgG (GE Healthcare Life Sciences) was used as the secondary Ab.…”

Section: Preparation Of Abs Against Vlse Epitopesmentioning

confidence: 99%

Epitope-Specific Evolution of Human B Cell Responses to Borrelia burgdorferi VlsE Protein from Early to Late Stages of Lyme Disease

Jacek

Tang

Komorowski

et al. 2016

The Journal of Immunology

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Most immunogenic proteins of Borrelia burgdorferi, the causative agent of Lyme disease, are known or expected to contain multiple B cell epitopes. However, the kinetics of the development of human B cell responses toward the various epitopes of individual proteins during the course of Lyme disease has not been examined. Using the highly immunogenic VlsE as a model Ag, we investigated the evolution of humoral immune responses toward its immunodominant sequences in 90 patients with a range of early to late manifestations of Lyme disease. The results demonstrate the existence of asynchronous, independently developing, Ab responses against the two major immunogenic regions of the VlsE molecule in the human host. Despite their strong immunogenicity, the target epitopes were inaccessible to Abs on intact spirochetes, suggesting a lack of direct immunoprotective effect. These observations document the association of immune reactivity toward specific VlsE sequences with different phases of Lyme disease, demonstrating the potential use of detailed epitope mapping of Ags for staging of the infection, and offer insights regarding the pathogen’s possible immune evasion mechanisms.

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Section: Preparation Of Abs Against Vlse Epitopesmentioning

confidence: 99%

Epitope-Specific Evolution of Human B Cell Responses to Borrelia burgdorferi VlsE Protein from Early to Late Stages of Lyme Disease

Jacek

Tang

Komorowski

et al. 2016

The Journal of Immunology

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“…During the past decade, it has been well established that CD is associated with various extraintestinal autoimmunities that involve the thyroid, joints, heart, skin, pancreas, bone, liver, reproductive organs, and the nervous system [38][39][40][41][42][43][44][45][46][47]. Although the exact mechanisms for the induction of these autoimmunities are not definitively known, there is a growing body of evidence indicating that these diseases may result from molecular mimicry between gliadin or transglutaminase and various tissue antigens, including nervous system proteins [8,[41][42][43]48].…”

Section: Cross-reaction Between α-Gliadin and Different Tissue Antigensmentioning

confidence: 99%

“…Although the exact mechanisms for the induction of these autoimmunities are not definitively known, there is a growing body of evidence indicating that these diseases may result from molecular mimicry between gliadin or transglutaminase and various tissue antigens, including nervous system proteins [8,[41][42][43]48]. Interestingly, the celiac peptide VVKVGGSSSLGW shares more than 30% homology with the transglutaminase peptide 476-487 (RIRVGQSMNMGS) [8].…”

Section: Cross-reaction Between α-Gliadin and Different Tissue Antigensmentioning

confidence: 99%

Cross-Reaction between Gliadin and Different Food and Tissue Antigens

Vojdani¹,

Tarash²

2013

FNS

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A subgroup of coeliac disease patients continues to experience symptoms even on a gluten-free diet (GFD). We attempted to determine whether these symptoms could be due to either cross-contamination with gluten-containing foods or cross-reactivity between α-gliadin and non-gluten foods consumed on a GFD. We measured the reactivity of affinity-purified polyclonal and monoclonal α-gliadin 33-mer peptide antibodies against gliadin and additional food antigens commonly consumed by patients on a GFD using ELISA and dot-blot. We also examined the immune reactivity of these antibodies with various tissue antigens. We observed significant immune reactivity when these antibodies were applied to cow's milk, milk chocolate, milk butyrophilin, whey protein, casein, yeast, oats, corn, millet, instant coffee and rice. To investigate whether there was cross-reactivity between α-gliadin antibody and different tissue antigens, we measured the degree to which this antibody bound to these antigens. The most significant binding occurred with asialoganglioside, hepatocyte, glutamic acid decarboxylase 65, adrenal 21-hydroxylase, and various neural antigens. The specificity of anti-α-gliadin binding to different food and tissue antigens was demonstrated by absorption and inhibition studies. We also observed significant cross-reactivity between α-gliadin 33-mer and various food antigens, but some of these reactions were associated with the contamination of non-gluten foods with traces of gluten. The consumption of cross-reactive foods as well as gluten-contaminated foods may be responsible for the continuing symptoms presented by a subgroup of patients with coeliac disease. The lack of response of some CD patients may also be due to antibody cross-reactivity with non-gliadin foods. These should then be treated as gluten-like peptides and should also be excluded from the diet when the GFD seems to fail.

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“…These include autoimmunity to the B peptide (amino acids 372 -395) of the glutamate/AMPA (a-3-hydroxy-5-methyl-4-isoxazolepropionic acid) subtype 3 receptor which may be associated with cross-reactivity to dsDNA or influenza A vaccination in patients with Rasmussens encephalitis. In addition, there are preliminary data showing cross-reactivity between gliadin and neuronal synapsin I in patients with celiac disease (which can be complicated by neurological syndromes such as neuropathy, seizures and behavioral changes) [157,162]. Finally, molecular mimicry may contribute to the pathogenesis of patients with APS that develop chorea [6,163].…”

Section: Chronic Neuroborreliosismentioning

confidence: 99%

Molecular mimicry in neurological disease: what is the evidence?

Lee

Levin

2008

Cell. Mol. Life Sci.

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Autoimmune diseases are a leading cause of disability and are increasing in incidence in industrialized countries. How people develop autoimmune diseases is not completely understood, but is related to an interaction between genetic background, environmental agents, autoantigens and the immune response. Molecular mimicry continues to be an important hypothesis that explains how an infection with an environmental agent results in autoimmune disease of the nervous system and other target organs. Although molecular mimicry has yet to be unequivocally proven, in the past several years there has been a sharpening of its definition with better experimental data implicating it as a cause of neurological disease in humans.

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Immune Cross-Reactivity in Celiac Disease: Anti-Gliadin Antibodies Bind to Neuronal Synapsin I

Cited by 99 publications

References 40 publications

Epitope-Specific Evolution of Human B Cell Responses to Borrelia burgdorferi VlsE Protein from Early to Late Stages of Lyme Disease

Epitope-Specific Evolution of Human B Cell Responses to Borrelia burgdorferi VlsE Protein from Early to Late Stages of Lyme Disease

Cross-Reaction between Gliadin and Different Food and Tissue Antigens

Molecular mimicry in neurological disease: what is the evidence?

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