Sialic Acid Receptors of Viruses

Matrosovich, Mikhail; Herrler, Georg; Klenk, Hans Dieter

doi:10.1007/128_2013_466

Cited by 232 publications

(280 citation statements)

References 198 publications

Supporting

Mentioning

262

Contrasting

Order By: Relevance

“…Influenza viruses bind to sialylated macromolecules, often with a preference for either a2,3-or a2,6-linked sialic acid (Matrosovich et al, 2013). Recognition of this linkage type may vary substantially depending on the context of the oligosaccharide containing this sugar in a terminal position (Sauer et al, 2014;Stevens et al, 2006).…”

Section: Discussionmentioning

confidence: 99%

Sialic acid-dependent interactions between influenza viruses and Streptococcus suis affect the infection of porcine tracheal cells

Meng

Seitz³

et al. 2015

Journal of General Virology

Self Cite

View full text Add to dashboard Cite

Section: Discussionmentioning

confidence: 99%

Sialic acid-dependent interactions between influenza viruses and Streptococcus suis affect the infection of porcine tracheal cells

Meng

Seitz³

et al. 2015

Journal of General Virology

Self Cite

View full text Add to dashboard Cite

“…Another ganglioside, GD1a, binds polyoma viruses, including the human pathogens, JC and BK viruses (14,15), and the E. coli toxin LT-IIB (60), and, like asialoGM1, can also function as a coreceptor for TLR2 (30). Another important class of respiratory pathogens, influenza viruses, bind to airway ECs through interaction of the viral HA protein with SA residues of glycoproteins and gangliosides (33). In the present studies, NEU3 was localized to superficial epithelia and the ciliated brush border (Fig.…”

Section: Discussionmentioning

confidence: 99%

“…The human airway epithelial surface is decorated with glycoconjugates expressing SA connected to underlying sugars in ␣-2,3 and ␣-2,6 linkages (12). These sialylated glycoconjugates include specific receptors that respond to danger signals (9), serve as binding sites for pathogenic bacteria and viruses (23,31,33), and initiate epithelial repair programs (9). Superimposed on this highly sialylated EC surface is a constantly moving, SA-rich mucous blanket (50).…”

mentioning

confidence: 99%

Human airway epithelia express catalytically active NEU3 sialidase

Lillehoj

Hyun²,

Feng

et al. 2014

American Journal of Physiology-Lung Cellular and Molecular Phys

View full text Add to dashboard Cite

acids on glycoconjugates play a pivotal role in many biological processes. In the airways, sialylated glycoproteins and glycolipids are strategically positioned on the plasma membranes of epithelia to regulate receptor-ligand, cell-cell, and host-pathogen interactions at the molecular level. We now demonstrate, for the first time, sialidase activity for ganglioside substrates in human airway epithelia. Of the four known mammalian sialidases, NEU3 has a substrate preference for gangliosides and is expressed at mRNA and protein levels at comparable abundance in epithelia derived from human trachea, bronchi, small airways, and alveoli. In small airway and alveolar epithelia, NEU3 protein was immunolocalized to the plasma membrane, cytosolic, and nuclear subcellular fractions. Small interfering RNA-induced silencing of NEU3 expression diminished sialidase activity for a ganglioside substrate by Ͼ70%. NEU3 immunostaining of intact human lung tissue could be localized to the superficial epithelia, including the ciliated brush border, as well as to nuclei. However, NEU3 was reduced in subepithelial tissues. These results indicate that human airway epithelia express catalytically active NEU3 sialidase.

show abstract

“…To date, several viruses, e.g. influenza virus or polyomaviruses, have been shown to bind specifically to sialic acid present on the surface of target cells, whilst its possible role in EHV-1 infection has not yet been described (Matrosovich et al, 2015). We found that removal of sialic acid residues from cells inhibited EHV-1 infection of CD172a + cells by 90-100 %.…”

Section: Discussionmentioning

confidence: 52%

Entry of equid herpesvirus 1 into CD172a+ monocytic cells

Laval

Favoreel

Cleemput

et al. 2016

Journal of General Virology

View full text Add to dashboard Cite

Equid herpesvirus 1 (EHV-1) causes respiratory disease, abortion and neurological disorders in horses. Cells from the myeloid lineage (CD172a In contrast, we found that treatment of cells with neuraminidase (NA) reduced infection by 85-100 % compared with untreated cells, whilst NA treatment of virus had no effect on infection. This shows that sialic acid residues present on CD172a + cells are essential in the initiation of EHV-1 infection. We found that a V b 3 integrins are involved in the post-binding stage of CD172a + cell infection. Using pharmacological inhibitors, we showed that EHV-1 does not enter CD172a + cells via a clathrin-or caveolae-dependent endocytic pathway, nor by macropinocytosis, but requires cholesterol, tyrosine kinase, actin, dynamin and endosomal acidification, pointing towards a phagocytic mechanism. Overall, these results show that the narrow tropism of EHV-1 amongst CD172a + cells is determined by the presence of specific cellular receptors.

show abstract

Sialic Acid Receptors of Viruses

Cited by 232 publications

References 198 publications

Sialic acid-dependent interactions between influenza viruses and Streptococcus suis affect the infection of porcine tracheal cells

Sialic acid-dependent interactions between influenza viruses and Streptococcus suis affect the infection of porcine tracheal cells

Human airway epithelia express catalytically active NEU3 sialidase

Entry of equid herpesvirus 1 into CD172a+ monocytic cells

Contact Info

Product

Resources

About