Medizinische Universität Graz Austria/Österreich - Forschungsportal - Medical University of Graz

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"Köpfe" der aktuellen Meldungen:

Ines Tawfik

Maria Anna Smolle

Teresa Gerhalter

Corina Madreiter-Sokolowski

Doris Eglseer

Samantha Hasenleithner

Diana Zabini-Polzer

Jelena Krstic

Elena Osto

Katrin Panzitt

Ruth Birner-Grünberger

Beate Rinner

Angelika Hofer

Barbara Obermayer-Pietsch

Marco Eigenfeld

Martin Zacharias

Paul Georg Gressenberger

Anirudh Subramanian Muralikrishnan

Nicolas Dominik Verheyen

Stephan Seiler

Christoph Augustin

Tobias Madl

Robert Sucher

Günther Silbernagel

Gabor Kovacs

Florian Singer

Martin Wagner

Andreas Prokesch

Christian Enzinger

Gernot Plank

Peter Fickert

Lorenzo Cerroni

Winfried März

Gewählte Publikation:

SHR Neuro Krebs Kardio Lipid Stoffw Microb

Cucco, A; Pearce, N; Simpson, A; Pembrey, L; Mpairwe, H; Figueiredo, CA; Cooper, PJ; Douwes, J; Brooks, C; Adcock, IM; Kermani, NZ; Roberts, GDM; Murray, CS; Custovic, A; Fontanella, S, , WASP, Study, Group;STELAR/UNICORN, Consortium;U-BIOPRED, Consortium, , WASP, Study, Group;STELAR/UNICORN, Consortium;U-BIOPRED, Consortium.
Exploring geographic differences in IgE response through network and manifold analyses.
J Allergy Clin Immunol. 2025; Doi: 10.1016/j.jaci.2025.05.032
PubMed FullText FullText_MUG

Autor*innen der Med Uni Graz:: Singer Florian
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Abstract:: BACKGROUND: Component-resolved diagnostics allow detailed assessment of IgE sensitization to multiple allergenic molecules (component-specific IgEs, or c-sIgEs) and may be useful for asthma diagnosis. However, to effectively use component-resolved diagnostics across diverse settings, it is crucial to account for geographic differences. OBJECTIVE: We investigated spatial determinants of c-sIgE networks to facilitate development of diagnostic algorithms applicable globally. METHODS: We used multiplex component-resolved diagnostics array to measure c-sIgE to 112 proteins in an international collaboration of several studies: WASP (World Asthma Phenotypes; United Kingdom, New Zealand, Brazil, Ecuador, and Uganda), U-BIOPRED (Unbiased Biomarkers for the Prediction of Respiratory Disease Outcomes; 7 European countries), and MAAS (Manchester Asthma and Allergy Study, a UK population-based birth cohort). Hierarchical clustering on low-dimensional representation of co-occurrence networks ascertained sensitization and c-sigE clusters across populations. Cross-country comparisons focused on a common subset of 18 c-sIgEs. We investigated sensitization networks across regions in relation to asthma severity. RESULTS: Sensitization profiles shared similarities across regions. For 18 c-sIgEs shared across study populations, the response structure enabled differentiation between different geographic areas and study designs, revealing 3 clusters: (1) Uganda, Ecuador, and Brazil, (2) U-BIOPRED children and adults, and (3) New Zealand, United Kingdom, and MAAS. Spectral clustering identified differences between clusters. We observed constant, almost parallel shifts between severe and nonsevere asthma in each country. CONCLUSIONS: Patterns of c-sIgE response reflect geographic location and study design. However, despite geographic differences in c-sIgE networks, there is a remarkably consistent shift between networks of subjects with nonsevere and severe asthma.