Abstract

BackgroundRespiratory syncytial virus (RSV) is a leading cause of bronchiolitis and pneumonia in young children worldwide, and no vaccine is currently available. Inactivated RSV vaccines tested in the 1960's led to vaccine-enhanced disease upon viral challenge, which has undermined RSV vaccine development. RSV infection is increasingly being recognized as an important pathogen in the elderly, as well as other individuals with compromised pulmonary immunity. A safe and effective inactivated RSV vaccine would be of tremendous therapeutic benefit to many of these populations.Principal FindingsIn these preclinical studies, a mouse model was utilized to assess the efficacy of a novel, nanoemulsion-adjuvanted, inactivated mucosal RSV vaccine. Our results demonstrate that NE-RSV immunization induced durable, RSV-specific humoral responses, both systemically and in the lungs. Vaccinated mice exhibited increased protection against subsequent live viral challenge, which was associated with an enhanced Th1/Th17 response. In these studies, NE-RSV vaccinated mice displayed no evidence of Th2 mediated immunopotentiation, as has been previously described for other inactivated RSV vaccines.ConclusionsThese studies indicate that nanoemulsion-based inactivated RSV vaccination can augment viral-specific immunity, decrease mucus production and increase viral clearance, without evidence of Th2 immune mediated pathology.

Highlights

  • Respiratory syncytial virus (RSV) infection is a major cause of respiratory illness, in infants

  • These studies indicate that nanoemulsion-based inactivated RSV vaccination can augment viral-specific immunity, decrease mucus production and increase viral clearance, without evidence of Th2 immune mediated pathology

  • While RSV is especially detrimental in very young infants whose airways are small and occluded, RSV is becoming recognized as an important pathogen in transplant recipients, the elderly, and patients with chronic lung diseases, especially chronic obstructive pulmonary disease (COPD) and asthma

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Summary

Introduction

Respiratory syncytial virus (RSV) infection is a major cause of respiratory illness, in infants. While RSV is especially detrimental in very young infants whose airways are small and occluded, RSV is becoming recognized as an important pathogen in transplant recipients, the elderly, and patients with chronic lung diseases, especially chronic obstructive pulmonary disease (COPD) and asthma. RSV is recognized as an important pathogen in the elderly and/or immunocompromised patients, and exacerbation of chronic lung disease. RSV causes severe lung disease in the young and the elderly. It is a problem in immunocompromised individuals, and is associated with significant mortality in these populations. RSV infection is increasingly being recognized as an important pathogen in the elderly, as well as other individuals with compromised pulmonary immunity. A safe and effective inactivated RSV vaccine would be of tremendous therapeutic benefit to many of these populations

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