B R Murphy scite author profile

To identify immunological predictors of resistance to influenza A infection and illness, the immunological status of live and inactivated virus vaccinees subsequently challenged with HlNl or H3N2 wild-type virus was examined. We refer to prechallenge antibodies of vaccinees receiving live attenuated virus as infection induced and those receiving inactivated virus as inactivated vaccine induced. Inactivated vaccine-induced protection against wild-type virus infection or illness correlated with the level of neuraminidase-inhibiting antibody in serum, local hemagglutinin immunoglobulin G (IgG) (but not IgA) enzyme-linked immunosorbent assay antibody, and hemagglutination-inhibiting antibody in serum. In contrast, infection-induced resistance to wild-type virus infection correlated with local hemagglutinin IgA antibody and neuraminidase-inhibiting antibody in serum, but not with hemagglutination-inhibiting antibody in serum. These observations suggest that live vaccine virus infection-induced and inactivated vaccine-induced immunity may involve different compartments of the immune system; sufficient antibody in either serum or nasal secretions is capable of conferring resistance.

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Human immune responses to influenza virus vaccines administered by systemic or mucosal routes

Moldoveanu

Clements

Prince

et al. 1995

Vaccine

176

113

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Advantage of Live Attenuated Cold-Adapted Influenza a Virus Over Inactivated Vaccine for a/Washington/80 (H3n2) Wild-Type Virus Infection

Clements¹,

Betts²,

Murphy³

1984

The Lancet

118

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Immunization of cotton rats with the fusion (F) and large (G) glycoproteins of respiratory syncytial virus (RSV) protects against RSV challenge without potentiating RSV disease

Murphy

Sotnikov

et al. 1989

Vaccine

102

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B R Murphy

Serum and nasal wash antibodies associated with resistance to experimental challenge with influenza A wild-type virus

Human immune responses to influenza virus vaccines administered by systemic or mucosal routes

Advantage of Live Attenuated Cold-Adapted Influenza a Virus Over Inactivated Vaccine for a/Washington/80 (H3n2) Wild-Type Virus Infection

Immunization of cotton rats with the fusion (F) and large (G) glycoproteins of respiratory syncytial virus (RSV) protects against RSV challenge without potentiating RSV disease

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