| Literature DB >> 30111851 |
Per Eriksson1, Cecilia Lindskog2, Ebbe Engholm3, Ola Blixt3, Jonas Waldenström4, Vincent Munster5, Åke Lundkvist1, Björn Olsen6, Elsa Jourdain7, Patrik Ellström8.
Abstract
Wild birds of Anseriformes and Charadriiformes are natural reservoirs of influenza A viruses (IAVs). Occasionally, IAVs transmit and adapt to mammalian hosts, and are maintained as epidemic strains in their new hosts. Viral adaptions to mammalian hosts include altered receptor preference of host epithelial sialylated oligosaccharides from terminal α2,3-linked sialic acid (SA) towards α2,6-linked SA. However, α2,3-linked SA has been found in human respiratory tract epithelium, and human infections by avian IAVs (AIVs) have been reported. To further explore the attachment properties of AIVs, four AIVs of different subtypes were investigated on human and pig tissues using virus histochemistry. Additionally, glycan array analysis was performed for further characterization of IAVs' receptor structure tropism. Generally, AIV attachment was more abundant to human tissues than to pig tissues. The attachment pattern was very strong to human conjunctiva and upper respiratory tract, but variable to the lower respiratory tract. AIVs mainly attached to α2,3-linked SA, but also to combinations of α2,3- and α2,6-linked SA. The low attachment of these AIV isolates to pig tissues, but high attachment to human tissues, addresses the question whether AIVs in general require passage through pigs to obtain adaptions towards mammalian receptor structures.Entities:
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Year: 2018 PMID: 30111851 PMCID: PMC6093914 DOI: 10.1038/s41598-018-29578-1
Source DB: PubMed Journal: Sci Rep ISSN: 2045-2322 Impact factor: 4.379
Figure 1Mean values of triplicate glycan PVA measurements. Error bars show plus/minus one standard deviation. The attachment signals were normalized towards the glycan with the highest virus attachment for each tested virus. Glycans 1–21 do not have any SA, glycans 22–37 all terminate with α2,3-linked SA, glycans 38–52 all terminate with α2,6-linked SA, and glycans 53–55 all carry multiple SAs.
Median scores of attachment of studied IAVs and lectins to human tissues.
| Tissue | Cell type | Human H3N2 | Mallard H3N2 | Mallard H6N1 | Turnstone H12N5 | Gull H16N3 | MAA-II | SNA | |||||||
|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|
| Score | n | Score | n | Score | n | Score | n | Score | n | Score | n | Score | n | ||
| Eye | Conjunctiva | −a | 2a | + | 3 | +a | 2a | + | 3 | +a | 2a | + | 1 | − | 1 |
| Cornea | −a | 3a | + | 4 | +a | 3a | + | 3 | +a | 3a | ± | 1 | − | 1 | |
| Nasopharynx | Ciliated | + | 4 | + | 9 | +a | 3a | + | 9 | +a | 4a | − | 8 | + | 8 |
| Goblet | + | 4 | + | 7 | +a | 3a | + | 7 | +a | 4a | − | 8 | + | 7 | |
| Bronchus | Ciliated | + | 4 | + | 5 | +a | 4a | ± | 5 | +a | 4a | − | 2 | + | 2 |
| Goblet | + | 4 | + | 4 | +a | 4a | ± | 4 | +a | 4a | − | 2 | + | 1 | |
| Lung | Pneumocytes | + | 4 | + | 10 | ±a | 4a | ± | 10 | +a | 4a | ± | 7 | + | 7 |
| Macrophages | − | 4 | + | 10 | ±a | 4a | ± | 10 | +a | 4a | ± | 5 | − | 7 | |
| Colon | Epithelial | −a | 4a | − | 6 | −a | 4a | − | 6 | −a | 4a | − | 5 | − | 5 |
| Goblet | −a | 4a | − | 6 | −a | 4a | − | 6 | −a | 4a | − | 5 | − | 5 | |
| Crypt | −a | 4a | − | 7 | −a | 4a | − | 7 | −a | 4a | − | 6 | − | 6 | |
Scoring key: −: <1% stained cells, ±: 1–50% stained cells, and +: >50% stained cells. n - number of tested individuals.
aValues were obtained from Lindskog et al.[23] after agreement with the authors and included to enable direct comparison[23].
Figure 2Attachment (in red) to human tissues of human H3N2, mallard H3N2, and ruddy turnstone H12N5 influenza viruses, as well as MAA-II and SNA lectins. The nuclei were counterstained with hematoxylin (blue). Panes showing human H3N2 virus staining of cornea, conjunctiva and colon were obtained from Lindskog et al.[23] after agreement with the authors and included to enable direct comparison[23].
Median scores of attachment of studied IAVs and lectins to pig tissues.
| Tissue | Cell type | Human H3N2 | Mallard H3N2 | Mallard H6N1 | Turnstone H12N5 | Gull H16N3 | MAA-II | SNA | |||||||
|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|
| Score | n | Score | n | Score | n | Score | n | Score | n | Score | n | Score | n | ||
| Trachea | Ciliated | ± | 5 | − | 5 | − | 5 | − | 4 | ± | 5 | − | 1 | + | 1 |
| Goblet | ± | 4 | − | 5 | − | 5 | − | 5 | − | 5 | − | 1 | + | 1 | |
| Bronchioles | Ciliated | + | 2 | − | 4 | − | 4 | − | 2 | − | 4 | − | 2 | + | 2 |
| Goblet | + | 2 | − | 4 | − | 4 | − | 2 | − | 4 | − | 2 | + | 1 | |
| Lung | Pneumocytes | − | 2 | ± | 4 | − | 4 | − | 2 | − | 4 | − | 2 | ± | 2 |
| Macrophages | − | 2 | ± | 4 | − | 4 | − | 2 | − | 4 | − | 2 | ± | 2 | |
Scoring key: −: <1% staining, ±: 1–50% staining, +: >50% staining, and N/A: not applicable. n - number of tested individuals.
Figure 3Attachment (in red) to pig tissues of human H3N2, mallard H3N2, mallard H6N1, ruddy turnstone H12N5, and black-headed gull H16N3 influenza viruses, as well as MAA-II and SNA lectins. The nuclei were counterstained with hematoxylin (blue).