Entry of the bat influenza H17N10 virus into mammalian cells is enabled by the MHC class II HLA-DR receptor.

Efstathios S Giotis George William Carnell Erik F Young Saleena S GhannyPatricia SoteropoulosLin-Fa WangWendy S BarclayMichael A SkinnerNigel Temperton

Published in: Nature microbiology (2019)

Haemagglutinin and neuraminidase surface glycoproteins of the bat influenza H17N10 virus neither bind to nor cleave sialic acid receptors, indicating that this virus employs cell entry mechanisms distinct from those of classical influenza A viruses. We observed that certain human haematopoietic cancer cell lines and canine MDCK II cells are susceptible to H17-pseudotyped viruses. We identified the human HLA-DR receptor as an entry mediator for H17 pseudotypes, suggesting that H17N10 possesses zoonotic potential.

Keyphrases

endothelial cells
induced pluripotent stem cells
induced apoptosis
pluripotent stem cells
papillary thyroid
single cell
editorial comment
young adults
squamous cell carcinoma
binding protein
squamous cell
human health
lymph node metastasis