Your search keyword '"Roberts Jr., Norbert J."' showing total 2 results

1. Human Alveolar Macrophages May Not Be Susceptible to Direct Infection by a Human Influenza Virus.

Author

Ettensohn, David B., Frampton, Mark W., Nichols, Joan E., Roberts Jr, Norbert J., and Roberts, Norbert J Jr

Subjects

ALVEOLAR macrophages, INFLUENZA viruses, VIRAL proteins, NEURAMINIDASE, FLUORESCEIN isothiocyanate, CELL culture, INFLUENZA, MACROPHAGES, VIRAL antibodies, VIRUSES, VIRAL physiology, INFLUENZA A virus, PHYSIOLOGY

Abstract

The current studies were undertaken to determine the susceptibility of human alveolar macrophages (AMs) to influenza A virus (IAV) infection in comparison with autologous peripheral blood-derived monocytes-macrophages (PBMs). AMs and PBMs were exposed to IAV in vitro and examined for their ability to bind and internalize IAV, and synthesize viral proteins and RNA. PBMs but not AMs demonstrated binding and internalization of the virus, synthesizing viral proteins and RNA. Exposure of AMs in the presence of a sialidase inhibitor or anti-IAV antibody resulted in viral protein synthesis by the cells. Exposure of AMs to fluorescein isothiocyanate-labeled IAV in the presence of anti-fluorescein isothiocyanate antibody also resulted in viral protein synthesis. Thus, human AMs are apparently not susceptible to direct infection by a human IAV but are likely to be infected indirectly in the setting of exposure in the presence of antibody that binds the challenging strain of IAV. [ABSTRACT FROM AUTHOR]

Published

2016

2. Respiratory Syncytial Virus F Envelope Protein Associates with Lipid Rafts without a Requirement for Other Virus Proteins.

Author

Fleming, Elisa H., Kolokoltsov, Andrey A., Davey, Robert A., Nichols, Joan E., and Roberts Jr., Norbert J.

Subjects

*VIRAL envelopes, *RESPIRATORY syncytial virus, *RECOMBINANT viruses, *VIRAL proteins, *PLASMIDS, *GENETIC vectors

Abstract

Like many enveloped viruses, human respiratory syncytial virus (RSV) assembles at and buds from lipid rafts. Translocation of the envelope proteins to these membrane subdomains is essential for production of infectious virus, but the targeting mechanism is poorly understood and it is not known if other virus proteins are required. Here we demonstrate that F protein of RSV intrinsically targets to lipid rafts without a requirement for any other virus protein, including the SH and G envelope proteins. Recombinant virus deficient in SH and G but retaining F protein expression was used to demonstrate that F protein still localized in rafts in both A549 and HEp-2 cells. Expression of a recombinant F gene by use of plasmid vectors demonstrated that F contains its own targeting domain and localized to rafts in the absence of other virus proteins. The domain responsible for translocation was then mapped. Unlike most other virus envelope proteins, F is unusual since the target signal is not contained within the cytoplasmic domain nor did it involve fatty acid modified residues. Furthermore, exchange of the transmembrane domain with that of the vesicular stomatitis virus G protein, a nonraft protein, did not alter F protein raft localization. Taken together, these data suggest that domains present in the extracellular portion of the protein are responsible for lipid raft targeting of the RSV F protein. [ABSTRACT FROM AUTHOR]

Published

2006