Morphology of subunits of respiratory syncytial (RS) virus

During the course of 26 respiratory syncytial (RS) virus infections, infected cells in the respiratory tract become coated with immunoglobulins (IgA, IgG, and IgM), IgA being predominant. Methods are described for detecting both intracellular virus and coating immunoglobulin using a double staining

## Abstract Human respiratory syncytial virus (RSV) is the major cause of lower respiratory tract disease in infants. It is unusual in that it causes repeated infections throughout life. Despite considerable efforts there is as yet no satisfactory vaccine available. This paper reviews the molecular

Human peripheral blood mononuclear cell (PBMC) proliferative responses to live respiratory syncytial (RS) virus, formalin-inactivated RS (FI-RS) virus, RS virus F (fusion) protein, and RS virus G (attachment) protein were assessed. All donors responded to challenge with whole RS virus antigens and F

## Abstract Lymphocyte proliferation assays were used to determine the ability of human and BALB/c T‐ lymphocytes to recognise and respond to in vitro challenge with purified preparations of four res piratory syncytial (RS) virus proteins. Human peripheral blood lymphocytes (PBLs) collected from ad

## Abstract A BALB/c model of respiratory syncytial virus infection has been developed in which hightitered replication occurs in lung, immunological infiltrates in lung can be detected histologically, and illness can be consistently reproduced. The immunodeterminants of RSV reinfection in this sys