1. Natural Resistance-Associated Macrophage Protein Is a Cellular Receptor for Sindbis Virus in Both Insect and Mammalian Hosts
- Author
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Nattha Wannissorn, Patrick P. Rose, Mark T. Heise, Anna Spiridigliozzi, Sara Cherry, Shelly Bambina, Susan R. Ross, Richard W. Hardy, Daniel P. Beiting, and Sheri L. Hanna
- Subjects
Sindbis virus ,Cancer Research ,Iron ,RNA Stability ,viruses ,Virus Attachment ,Alphavirus ,Transfection ,Microbiology ,Virus ,Article ,Cell Line ,Mice ,03 medical and health sciences ,Viral entry ,Virology ,Immunology and Microbiology(all) ,medicine ,Animals ,Drosophila Proteins ,Humans ,Immunoprecipitation ,Biotinylation ,Alphavirus infection ,Cation Transport Proteins ,Molecular Biology ,030304 developmental biology ,Host factor ,Mammals ,Host cell surface ,0303 health sciences ,biology ,Alphavirus Infections ,030306 microbiology ,fungi ,Vesiculovirus ,Virus Internalization ,biology.organism_classification ,medicine.disease ,3. Good health ,Culicidae ,Receptors, Virus ,Drosophila ,RNA Interference ,Parasitology ,Sindbis Virus ,West Nile virus ,Drosophila Protein - Abstract
SummaryAlphaviruses, including several emerging human pathogens, are a large family of mosquito-borne viruses with Sindbis virus being a prototypical member of the genus. The host factor requirements and receptors for entry of this class of viruses remain obscure. Using a Drosophila system, we identified the divalent metal ion transporter natural resistance-associated macrophage protein (NRAMP) as a host cell surface molecule required for Sindbis virus binding and entry into Drosophila cells. Consequently, flies mutant for dNRAMP were protected from virus infection. NRAMP2, the ubiquitously expressed vertebrate homolog, mediated binding and infection of Sindbis virus into mammalian cells, and murine cells deficient for NRAMP2 were nonpermissive to infection. Alphavirus glycoprotein chimeras demonstrated that the requirement for NRAMP2 is at the level of Sindbis virus entry. Given the conserved structure of alphavirus glycoproteins, and the widespread use of transporters for viral entry, other alphaviruses may use conserved multipass membrane proteins for infection.
- Published
- 2011
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