Protein N-glycosylation in the bronchoalveolar space differs between never-smokers and long-term smokers with and without COPD

Author:

Venkatakrishnan Vignesh12ORCID,Thomsson Kristina A12ORCID,Padra Médea12ORCID,Andersson Anders34ORCID,Brundin Bettina5,Christenson Karin67ORCID,Bylund Johan67ORCID,Karlsson Niclas G12ORCID,Lindén Anders589ORCID,Lindén Sara K12ORCID

Affiliation:

1. Department of Medical Chemistry and Cell Biology , Institute of Biomedicine, Sahlgrenska Academy, , Medicinaregatan 9C, 41390, Gothenburg, Sweden

2. University of Gothenburg , Institute of Biomedicine, Sahlgrenska Academy, , Medicinaregatan 9C, 41390, Gothenburg, Sweden

3. Institute of Medicine , Sahlgrenska Academy, , Medicinaregatan 3, 41390, Gothenburg, Sweden

4. University of Gothenburg , Sahlgrenska Academy, , Medicinaregatan 3, 41390, Gothenburg, Sweden

5. Division of Lung and Airway Research, Institute of Environmental Medicine, Karolinska Institutet , Nobels väg 13, 17177, Stockholm, Sweden

6. Department of Oral Microbiology and Immunology , Institute of Odontology, Sahlgrenska Academy, , Medicinaregatan 12F, 41390, Gothenburg, Sweden

7. University of Gothenburg , Institute of Odontology, Sahlgrenska Academy, , Medicinaregatan 12F, 41390, Gothenburg, Sweden

8. Department Respiratory Medicine and Allergy , Karolinska Severe COPD Center, , Solna, Eugeniavägen 3, 171 76 Stockholm, Sweden

9. Karolinska University Hospital , Karolinska Severe COPD Center, , Solna, Eugeniavägen 3, 171 76 Stockholm, Sweden

Abstract

Abstract Chronic obstructive pulmonary disease (COPD) kills millions of people annually and patients suffering from exacerbations of this disorder display high morbidity and mortality. The clinical course of COPD is associated with dysbiosis and infections, but the underlying mechanisms are poorly understood. Glycosylation of proteins play roles in regulating interactions between microbes and immune cells, and knowledge on airway glycans therefore contribute to the understanding of infections. Furthermore, glycans have biomarker potential for identifying smokers with enhanced risk for developing COPD as well as COPD subgroups. Here, we characterized the N-glycosylation in the lower airways of healthy never-smokers (HNS, n = 5) and long-term smokers (LTS) with (LTS+, n = 4) and without COPD (LTS−, n = 8). Using mass spectrometry, we identified 57 highly confident N-glycan structures whereof 38 oligomannose, complex, and paucimannose type glycans were common to BAL samples from HNS, LTS− and LTS+ groups. Hybrid type N-glycans were identified only in the LTS+ group. Qualitatively and quantitatively, HNS had lower inter-individual variation between samples compared to LTS− or LTS+. Cluster analysis of BAL N-glycosylation distinguished LTS from HNS. Correlation analysis with clinical parameters revealed that complex N-glycans were associated with health and absence of smoking whereas oligomannose N-glycans were associated with smoking and disease. The N-glycan profile from monocyte-derived macrophages differed from the BAL N-glycan profiles. In conclusion, long-term smokers display substantial alterations of N-glycosylation in the bronchoalveolar space, and the hybrid N-glycans identified only in long-term smokers with COPD deserve to be further studied as potential biomarkers.

Funder

Swedish Research Council

Swedish Heart-Lung Foundation

Australian Liver Foundation

Västra Götaland Region

Region Stockholm

Publisher

Oxford University Press (OUP)

Subject

Biochemistry

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