In a murine model of respiratory syncytial virus disease, prior sensitization to the attachment glycoprotein (G) leads to pulmonary eosinophilia and enhanced illness. Three different approaches were taken to dissect the region of G responsible for enhanced disease and protection against challenge. First, mutant viruses, containing frameshifts that altered the COOH terminus of the G protein, were used to challenge mice sensitized by scarification with recombinant vaccinia virus (rVV) expressing wild-type G. Second, cDNA expressing these mutated G proteins were expressed by rVV and used to vaccinate mice before challenge with wild-type respiratory syncytial virus (RSV). These studies identified residues 193–205 to be responsible for G-induced weight loss and lung eosinophilia and showed that this region was not was not necessary for induction of protective immunity. Third, mice were sensitized using an rVV that expressed only amino acids 124–203 of the G protein. Upon RSV challenge, mice sensitized with this rVV developed enhanced weight loss and eosinophilia. This is the first time that a region within RSV (amino acids 193–203) has been shown to be responsible for induction of lung eosinophilia and disease enhancement. Moreover, we now show that it is possible to induce protective immunity with an altered G protein without inducing a pathological response.
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1 June 1998
Brief Definitive Report|
June 01 1998
Eliminating a Region of Respiratory Syncytial Virus Attachment Protein Allows Induction of Protective Immunity without Vaccine-enhanced Lung Eosinophilia
Tim E. Sparer,
Tim E. Sparer
From the *Imperial College School of Medicine, National Heart and Lung Institute at St. Mary's, London, W2 1PG United Kingdom; and the ‡Centro Nacional de Biologìa Celular y Retrovirus, Instituto de Salud ‘Carlos III', Majadahonda, 28220, Madrid, Spain
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Stephen Matthews,
Stephen Matthews
From the *Imperial College School of Medicine, National Heart and Lung Institute at St. Mary's, London, W2 1PG United Kingdom; and the ‡Centro Nacional de Biologìa Celular y Retrovirus, Instituto de Salud ‘Carlos III', Majadahonda, 28220, Madrid, Spain
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Tracy Hussell,
Tracy Hussell
From the *Imperial College School of Medicine, National Heart and Lung Institute at St. Mary's, London, W2 1PG United Kingdom; and the ‡Centro Nacional de Biologìa Celular y Retrovirus, Instituto de Salud ‘Carlos III', Majadahonda, 28220, Madrid, Spain
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Aaron J. Rae,
Aaron J. Rae
From the *Imperial College School of Medicine, National Heart and Lung Institute at St. Mary's, London, W2 1PG United Kingdom; and the ‡Centro Nacional de Biologìa Celular y Retrovirus, Instituto de Salud ‘Carlos III', Majadahonda, 28220, Madrid, Spain
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Blanca Garcia-Barreno,
Blanca Garcia-Barreno
From the *Imperial College School of Medicine, National Heart and Lung Institute at St. Mary's, London, W2 1PG United Kingdom; and the ‡Centro Nacional de Biologìa Celular y Retrovirus, Instituto de Salud ‘Carlos III', Majadahonda, 28220, Madrid, Spain
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Jose A. Melero,
Jose A. Melero
From the *Imperial College School of Medicine, National Heart and Lung Institute at St. Mary's, London, W2 1PG United Kingdom; and the ‡Centro Nacional de Biologìa Celular y Retrovirus, Instituto de Salud ‘Carlos III', Majadahonda, 28220, Madrid, Spain
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Peter J.M. Openshaw
Peter J.M. Openshaw
From the *Imperial College School of Medicine, National Heart and Lung Institute at St. Mary's, London, W2 1PG United Kingdom; and the ‡Centro Nacional de Biologìa Celular y Retrovirus, Instituto de Salud ‘Carlos III', Majadahonda, 28220, Madrid, Spain
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Tim E. Sparer
From the *Imperial College School of Medicine, National Heart and Lung Institute at St. Mary's, London, W2 1PG United Kingdom; and the ‡Centro Nacional de Biologìa Celular y Retrovirus, Instituto de Salud ‘Carlos III', Majadahonda, 28220, Madrid, Spain
Stephen Matthews
From the *Imperial College School of Medicine, National Heart and Lung Institute at St. Mary's, London, W2 1PG United Kingdom; and the ‡Centro Nacional de Biologìa Celular y Retrovirus, Instituto de Salud ‘Carlos III', Majadahonda, 28220, Madrid, Spain
Tracy Hussell
From the *Imperial College School of Medicine, National Heart and Lung Institute at St. Mary's, London, W2 1PG United Kingdom; and the ‡Centro Nacional de Biologìa Celular y Retrovirus, Instituto de Salud ‘Carlos III', Majadahonda, 28220, Madrid, Spain
Aaron J. Rae
From the *Imperial College School of Medicine, National Heart and Lung Institute at St. Mary's, London, W2 1PG United Kingdom; and the ‡Centro Nacional de Biologìa Celular y Retrovirus, Instituto de Salud ‘Carlos III', Majadahonda, 28220, Madrid, Spain
Blanca Garcia-Barreno
From the *Imperial College School of Medicine, National Heart and Lung Institute at St. Mary's, London, W2 1PG United Kingdom; and the ‡Centro Nacional de Biologìa Celular y Retrovirus, Instituto de Salud ‘Carlos III', Majadahonda, 28220, Madrid, Spain
Jose A. Melero
From the *Imperial College School of Medicine, National Heart and Lung Institute at St. Mary's, London, W2 1PG United Kingdom; and the ‡Centro Nacional de Biologìa Celular y Retrovirus, Instituto de Salud ‘Carlos III', Majadahonda, 28220, Madrid, Spain
Peter J.M. Openshaw
From the *Imperial College School of Medicine, National Heart and Lung Institute at St. Mary's, London, W2 1PG United Kingdom; and the ‡Centro Nacional de Biologìa Celular y Retrovirus, Instituto de Salud ‘Carlos III', Majadahonda, 28220, Madrid, Spain
Address correspondence to Peter Openshaw, Imperial College School of Medicine, National Heart and Lung Institute at St. Mary's, Norfolk Place, London, W2 1PG United Kingdom. Phone: 44-0171-594-3854; Fax: 44-0171-724-7349; E-mail: [email protected]
T.E. Sparer and S. Matthews contributed equally to this work.
Received:
December 26 1997
Revision Received:
March 18 1998
Online ISSN: 1540-9538
Print ISSN: 0022-1007
1998
J Exp Med (1998) 187 (11): 1921–1926.
Article history
Received:
December 26 1997
Revision Received:
March 18 1998
Citation
Tim E. Sparer, Stephen Matthews, Tracy Hussell, Aaron J. Rae, Blanca Garcia-Barreno, Jose A. Melero, Peter J.M. Openshaw; Eliminating a Region of Respiratory Syncytial Virus Attachment Protein Allows Induction of Protective Immunity without Vaccine-enhanced Lung Eosinophilia . J Exp Med 1 June 1998; 187 (11): 1921–1926. doi: https://doi.org/10.1084/jem.187.11.1921
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