Patients With Atopic Dermatitis Sensitized to Pet Dander Mount IgE and T-Cell Responses to Mammalian Cystatins, Including the Human Self-Protein

Roesner, Lennart M.; Swiontek, Kyra; Lentz, Delphine; Begemann, Gabriele; Kienlin, Petra; Hentges, François; Ollert, Markus; Werfel, T.; Hilger, Christiane

doi:10.18176/jiaci.0737

Cited by 4 publications

(6 citation statements)

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“…Nevertheless, these results might also indicate a need for the identification of new molecular allergens to which current non‐sensitized individuals might be sensitized 16,24 . Two new dog allergen molecules, Can f 7 and Can f 8, have been recently identified and added to the WHO/IUIS Allergen Nomenclature database, after the analyses in our study and the study by Käck and colleagues were performed 18,39,40 . Another explanation could be the presence of α‐Gal in cat and dog dander extracts 41 .…”

Section: Discussionmentioning

confidence: 75%

“… 16 , 24 Two new dog allergen molecules, Can f 7 and Can f 8, have been recently identified and added to the WHO/IUIS Allergen Nomenclature database, after the analyses in our study and the study by Käck and colleagues were performed. 18 , 39 , 40 Another explanation could be the presence of α‐Gal in cat and dog dander extracts. 41 Kiewiet et al, 42 in a recent study of patients with α‐Gal syndrome, found a high frequency of sensitization to both dog and cat extracts but a low frequency of genuine cat and dog sensitization using CRD.…”

Section: Discussionmentioning

confidence: 99%

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Sensitization to molecular dog allergens in an adult population: Results from the West Sweden Asthma Study

Ermis

Borres

Basna

et al. 2022

Clin Experimental Allergy

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Background: As the prevalence of dog allergy rises, component resolved diagnosis might improve the diagnosis, understanding of the clinical outcomes and the effectiveness of immunotherapy. Considering the paucity of data in adults, the current study characterized the patterns of sensitization to dog molecular allergens in an adult population. Methods: Data were derived from the West Sweden Asthma Study, a populationbased and representative sample of adults from western Sweden. Of the 2006 subjects clinically examined, 313 participants sensitized to whole dog allergen extract were measured for specific immunoglobulin E (sIgE) levels to Can f 1, Can f 2, Can f 3, Can f 4, Can f 5 and Can f 6 using ImmunoCAP™. Polysensitization was defined as sensitization to ≥3 components. Overlapping sensitization was defined as having concomitant sensitization to at least two dog molecular allergen families (lipocalin, albumin or prostatic kallikrein).Results: Of 313, 218 (70%) subjects tested positive to at least one dog allergen component. Sensitization to Can f 1 (43%) was the most common, followed by Can f 5 (33%) among molecular allergens, while sensitization to lipocalins (56%) was the most common among component families. Polysensitization was found in 22% of all participants and was more common in participants with than in those without asthma.Subjects with asthma were less likely to be monosensitized to Can f 5 than those without asthma. Subjects with asthma had higher IgE levels of Can f 3, Can f 4 and | ME THODS | Study participantsThe study data were derived from an ongoing population-based longitudinal study, the West Sweden Asthma Study (WSAS). Details of the study procedures have been described elsewhere. 25,26 We sent out 30,000 postal questionnaires to randomly selected 16-75-year-old adults living in the Västra Götaland region of Can f 6 than those without asthma. Overlapping sensitizations also differed between those with asthma and allergic rhinitis and those without. Conclusion:Increased knowledge about the sensitization patterns of dog allergen components can aid in defining their role in asthma and rhinitis. In complex clinical cases of dog allergy, a detailed analysis of dog allergen components can provide additional information on the nature of sensitization. K E Y W O R D Scomponent resolved diagnostics, dog allergy, dog dander sensitization, dog molecular allergen components, furry animal allergy, Can f 1, Can f 5 Key Message• Can f 1 (43%) and Can f 5 (33%) were the most commonly sensitized single components.

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Section: Discussionmentioning

confidence: 75%

Section: Discussionmentioning

confidence: 99%

Sensitization to molecular dog allergens in an adult population: Results from the West Sweden Asthma Study

Ermis

Borres

Basna

et al. 2022

Clin Experimental Allergy

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“…These autoantigens may then be processed by antigen presenting cells and presented to lymphocytes resulting in the production of IgG and/or IgE AAb by plasma cells 105 . IgE‐mediated autoimmunity in AD may also be caused by molecular mimicry due to cross‐reactive peptides between environmental antigens or skin microbiome and self‐antigens 91,106–108 . In addition, skin residing CD8 + cytotoxic T cells with intermediate affinity to self‐peptides may contribute to skin damage, and unconventional γδ T cells may also accumulate in the skin 109,110 .…”

Section: Autoreactive Ige In Atopic Dermatitismentioning

confidence: 99%

“…105 IgE-mediated autoimmunity in AD may also be caused by molecular mimicry due to cross-reactive peptides between environmental antigens or skin microbiome and self-antigens. 91,[106][107][108] In addition, skin residing CD8 + cytotoxic T cells with intermediate affinity to self-peptides may contribute to skin damage, and unconventional γδ T cells may also accumulate in the skin. 109,110 Finally, an extraordinary unspecific activation of the T and B cells might also underlie the response due to the conditions of an ongoing inflammation.…”

Section: Autore Ac Tive I G E In Atopi C Dermatitismentioning

confidence: 99%

Autoreactive IgE: Pathogenic role and therapeutic target in autoimmune diseases

Charles

Krohn

Kocatürk

et al. 2023

Allergy

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Autoimmunity is the break of tolerance to self‐antigens that leads to organ‐specific or systemic diseases often characterized by the presence of pathogenic autoreactive antibodies (AAb) produced by plasmablast and/or plasma cells. AAb are prevalent in the general population and not systematically associated with clinical symptoms. In contrast, in some individuals, these AAb are pathogenic and drive the development of signs and symptoms of antibody‐mediated autoimmune diseases (AbAID). AAb production, isotype profiles, and glycosylations are promoted by pro‐inflammatory triggers linked to genetic, environmental, and hormonal parameters. Recent evidence supports a role for pathogenic AAb of the IgE isotype in a number of AbAID. Autoreactive IgE can drive the activation of mast cells, basophils, and other types of FcεRI‐bearing cells and may play a role in promoting autoantibody production and other pro‐inflammatory pathways. In this review, we discuss the current knowledge on the pathogenicity of autoreactive IgE in AbAID and their status as therapeutic targets. We also highlight unresolved issues including the need for assays that reproducibly quantify IgE AAbs, to validate their diagnostic and prognostic value, and to further study their pathophysiological contributions to AbAID.

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“…These autoantigens may then be processed by antigen presenting cells and presented to lymphocytes resulting in the production of IgG and/or IgE AAb by plasma cells 103 . IgE-mediated autoimmunity in AD may also be caused by molecular mimicry due to cross-reactive peptides between environmental antigens or skin microbiome and self-antigens 89,[104][105][106] . In addition, skin residing CD8 + cytotoxic T cells with intermediate affinity to selfpeptides may contribute to skin damage, and unconventional γδ T cells may also accumulate in the skin 107,108 .…”

Section: Introductionmentioning

confidence: 99%

Autoreactive IgE: pathogenic role and therapeutic target in autoimmune diseases

Charles

Krohn

Kocatürk

et al. 2023

Preprint

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Autoimmunity is the break of tolerance to self-antigens that leads to organ-specific or systemic diseases characterized by the presence of pathogenic autoreactive antibodies (AAb) produced by plasmablast and/or plasma cells. AAb are prevalent in the general population and not systematically associated with clinical symptoms. In contrast, in some individuals, these AAb are pathogenic and drive the development of signs and symptoms of antibody-mediated autoimmune diseases (AbAID). AAb production, isotype profiles, and glycosylations are promoted by pro-inflammatory triggers linked to genetic, environmental, and hormonal parameters. Recent evidence supports a role for pathogenic AAb of the IgE isotype in a number of AbAID. Autoreactive IgE can drive the activation of mast cells, basophils and other types of FcεRI-bearing cells and may play a role in promoting autoantibody production and other pro-inflammatory pathways. In this review, we discuss the current knowledge on the pathogenicity of autoreactive IgE in AbAID and their status as therapeutic targets. We also highlight unresolved issues including the need for assays that reproducibly quantify IgE AAbs, to validate their diagnostic and prognostic value, and to further study their pathophysiological contributions to AbAID.

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Patients With Atopic Dermatitis Sensitized to Pet Dander Mount IgE and T-Cell Responses to Mammalian Cystatins, Including the Human Self-Protein

Cited by 4 publications

References 0 publications

Sensitization to molecular dog allergens in an adult population: Results from the West Sweden Asthma Study

Sensitization to molecular dog allergens in an adult population: Results from the West Sweden Asthma Study

Autoreactive IgE: Pathogenic role and therapeutic target in autoimmune diseases

Autoreactive IgE: pathogenic role and therapeutic target in autoimmune diseases

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