A novel non-invasive method allowing for discovery of pathologically relevant proteins from small airways.

Clin Proteomics

Occupational and Environmental Medicine, Department of Public Health and Community Medicine, Institute of Medicine, Sahlgrenska Academy, University of Gothenburg, Gothenburg, Sweden.

Published: June 2022

AI Article Synopsis

  • There is an urgent need for accurate biomarkers in respiratory medicine, particularly for small airway pathology, which can be assessed through the PExA method that collects aerosol droplet particles from breath.
  • The study examined a group of healthy individuals and asthma patients, finding 207 proteins in the samples, with nine proteins showing significant differences in abundance related to asthma severity.
  • The findings suggest that PExA-derived proteomics could serve as a valuable tool for exploring biomarkers in respiratory diseases, potentially leading to personalized medicine advancements.

Article Abstract

Background: There is a lack of early and precise biomarkers for personalized respiratory medicine. Breath contains an aerosol of droplet particles, which are formed from the epithelial lining fluid when the small airways close and re-open during inhalation succeeding a full expiration. These particles can be collected by impaction using the PExA method (Particles in Exhaled Air), and are derived from an area of high clinical interest previously difficult to access, making them a potential source of biomarkers reflecting pathological processes in the small airways.

Research Question: Our aim was to investigate if PExA method is useful for discovery of biomarkers that reflect pathology of small airways.

Methods And Analysis: Ten healthy controls and 20 subjects with asthma, of whom 10 with small airway involvement as indicated by a high lung clearance index (LCI ≥ 2.9 z-score), were examined in a cross-sectional design, using the PExA instrument. The samples were analysed with the SOMAscan proteomics platform (SomaLogic Inc.).

Results: Two hundred-seven proteins were detected in up to 80% of the samples. Nine proteins showed differential abundance in subjects with asthma and high LCI as compared to healthy controls. Two of these were less abundant (ALDOA4, C4), and seven more abundant (FIGF, SERPINA1, CD93, CCL18, F10, IgM, IL1RAP). sRAGE levels were lower in ex-smokers (n = 14) than in never smokers (n = 16). Gene Ontology (GO) annotation database analyses revealed that the PEx proteome is enriched in extracellular proteins associated with extracellular exosome-vesicles and innate immunity.

Conclusion: The applied analytical method was reproducible and allowed identification of pathologically interesting proteins in PEx samples from asthmatic subjects with high LCI. The results suggest that PEx based proteomics is a novel and promising approach to study respiratory diseases with small airway involvement.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9167914PMC
http://dx.doi.org/10.1186/s12014-022-09348-yDOI Listing

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