Cytotoxic T Lymphocytes Established by Seasonal Human Influenza Cross-React against 2009 Pandemic H1N1 Influenza Virus

Tu, Wenwei; Mao, Huawei; Zheng, Jian; Liu, Yinping; Chiu, Susan S.; Qin, Gang; Chan, Ping-Lung; Lam, Kwok-Tai; Guan, Jing; Zhang, Lijuan; Guan, Yi; Yuen, Kwok‐Yung; Peiris, Malik; Lau, Yu‐Lung

doi:10.1128/jvi.00519-10

Cited by 138 publications

(136 citation statements)

References 59 publications

(105 reference statements)

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“…These results suggest that CD4 + T-cell epitopes are shared between the ca and WT viruses. Our data are consistent with reports by others (18)(19)(20) including Greenbaum et al that up to 41% of CD4 + T-cell epitopes are conserved between seasonal and 2009 p-H1N1 in humans and that these epitopes are mainly located in the internal protein genes.…”

Section: Elisa Antibodysupporting

confidence: 83%

“…The transmission of the p-H1N1 virus was reduced when guinea pigs were previously infected with seasonal H1N1 or H3N2 influenza viruses (17). Recent studies examining the molecular basis for preexisting immunity to the p-H1N1 virus have demonstrated that a number of CD4 and CD8 T epitopes (18)(19)(20) are shared between the pandemic and seasonal H1N1 viruses. Studies on the effect of seasonal influenza vaccination have had discrepant results: Ferrets that were vaccinated with seasonal trivalent inactivated vaccine (s-TIV) before receipt of an adjuvanted p-H1N1 vaccine developed higher antibody titers than animals that were not primed; however, despite the difference in antibody titer, no difference in protective efficacy was observed (21).…”

mentioning

confidence: 99%

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Seasonal influenza infection and live vaccine prime for a response to the 2009 pandemic H1N1 vaccine

Chen

Lau

Lamirande

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

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The robust immune response to a single dose of pandemic 2009 H1N1 vaccine suggests that a large segment of the population has been previously primed. We evaluated the effect of seasonal (s) H1N1 infection, s-trivalent inactivated vaccine (s-TIV), and trivalent s-live attenuated influenza vaccine (s-LAIV) before immunization with a pandemic live attenuated influenza vaccine (p-LAIV) in mice. We compared serum and mucosal antibody and pulmonary CD8 and CD4 responses and the virologic response to challenge with a wild-type 2009 pandemic H1N1 (p-H1N1) virus. Two doses of p-LAIV induced cellular immune and robust ELISA and neutralizing antibody responses that were associated with complete protection from p-H1N1 challenge. A single dose of p-LAIV induced a cellular response and ELISA but not a neutralizing antibody response, and incomplete protection from p-H1N1 virus challenge. Primary infection with s-H1N1 influenza virus followed by a dose of p-LAIV resulted in cross-reactive ELISA antibodies and a robust cellular immune response that was also associated with complete protection from p-H1N1 virus challenge. A lower-magnitude but similar response associated with partial protection was seen in mice that received a dose of s-LAIV followed by p-LAIV. Mice that received a dose of s-TIV followed by p-LAIV did not show any evidence of priming. In summary, prior infection with a seasonal influenza virus or s-LAIV primed mice for a robust response to a single dose of p-LAIV that was associated with protection equivalent to two doses of the matched pandemic vaccine.

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Section: Elisa Antibodysupporting

confidence: 83%

mentioning

confidence: 99%

Seasonal influenza infection and live vaccine prime for a response to the 2009 pandemic H1N1 vaccine

Chen

Lau

Lamirande

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

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“…Therefore, an important consideration in evaluating candidate vaccines should be the degree to which they elicit crossreactive cell-mediated immunity. Although influenza-specific T cells do not provide sterilizing immunity, they protect more broadly than neutralizing antibodies against heterologous and heterosubtypic strains through viral clearance [10,11]. Broadly cross-reactive T cell epitopes are typically located in internal proteins of influenza viruses such as the nucleoprotein (NP) and matrix (M1) segments, which are more conserved than the surface hemagglutinin (HA) and NA glycoproteins [12][13][14].…”

Section: Introductionmentioning

confidence: 99%

Vaccination with NS1-truncated H3N2 swine influenza virus primes T cells and confers cross-protection against an H1N1 heterosubtypic challenge in pigs

Kappes

Sandbulte

Platt

et al. 2012

Vaccine

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The diversity of contemporary swine influenza virus (SIV) strains impedes effective immunization of swine herds. Mucosally delivered, attenuated virus vaccines are one approach with potential to provide broad crossprotection. Reverse genetics-derived H3N2 SIV virus with truncated NS1 (NS1Δ126 TX98) is attenuated and immunogenic when delivered intranasally in young pigs. We analyzed T-cell priming and cross-protective efficacy in weanling piglets after intranasal inoculation with NS1Δ126 TX98 versus wild type TX98. In vivo replication of the truncation mutant was minimal compared to the wild type virus. T-cell responses were greater in magnitude in pigs infected with the wild type virus in in vitro restimulation assays. According to the expression of activation marker CD25, peripheral T cell recall responses in NS1Δ126 TX98 infected pigs were minimal. However, intracellular IFN-γ data indicate that the attenuated virus induced virus-specific CD4 + CD8 -, CD4 + CD8 + , CD4 -CD8 + , and γδ T cells within 28 days. The IFN-γ response appeared to contract, as responses were reduced at later time points prior to challenge. CD4 + CD8 + cells isolated 5 days after heterosubtypic H1N1 challenge (day 70 overall) showed an elevated CD25 response to virus restimulation. Pigs previously infected with wild type TX98 were protected from replication of the H1N1 challenge virus. Vaccination with NS1Δ126 TX98 was associated with significantly lower levels of Th1-associated cytokines in infected lungs but provided partial cross-protection against the H1N1 challenge. These results demonstrate that NS1Δ SIV vaccines can elicit cell-mediated cross-protection against antigenically divergent strains. The diversity of contemporary swine influenza virus (SIV) strains impedes effective immunization of swine herds. Mucosally delivered, attenuated virus vaccines are one approach with potential to provide broad cross-protection. Reverse genetics-derived H3N2 SIV virus with truncated NS1 (NS1 126 TX98) is attenuated and immunogenic when delivered intranasally in young pigs. We analyzed T-cell priming and cross-protective efficacy in weanling piglets after intranasal inoculation with NS1 126 TX98 versus wild type TX98. In vivo replication of the truncation mutant was minimal compared to the wild type virus. T-cell responses were greater in magnitude in pigs infected with the wild type virus in in vitro restimulation assays. According to the expression of activation marker CD25, peripheral T cell recall responses in NS1 126 TX98 infected pigs were minimal. However, intracellular IFN-␥ data indicate that the attenuated virus induced virus-specific CD4 + CD8 -, CD4 + CD8 + , CD4 -CD8 + , and ␥␦ T cells within 28 days. The IFN-␥ response appeared to contract, as responses were reduced at later time points prior to challenge. CD4 + CD8 + cells isolated 5 days after heterosubtypic H1N1 challenge (day 70 overall) showed an elevated CD25 response to virus restimulation. Pigs previously infected with wild type TX98 were protected from replicatio...

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“…Since human T-cells specific for seasonal IAVs also display strong cross-reactivity with IAVs of other subtypes (Jameson et al, 1999;Kreijtz et al, 2008;Lee et al, 2008) and pH1N1 2009 viruses (Richards et al, 2010;Tu et al, 2010), it can be hypothesized that individuals with a history of IAV infection were protected from pH1N1 virus infections to a certain extent. This would imply that young children that are supposedly immunologically naïve for IAV would be more at risk for developing severe disease.…”

Section: T-cells Provide Protection Against Infection With Ph1n1mentioning

confidence: 99%

Cross-protective immunity against influenza pH1N1 2009 viruses induced by seasonal influenza A (H3N2) virus is mediated by virus-specific T-cells

Hillaire

Trierum

Kreijtz

et al. 2011

Journal of General Virology

107

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Influenza A (H1N1) viruses of swine origin were introduced into the human population in 2009 and caused a pandemic. The disease burden in the elderly was relatively low, which was attributed to the presence of cross-reacting serum antibodies in this age group, which were raised against seasonal influenza A (H1N1) viruses that circulated before 1957. It has also been described how infection with heterosubtypic influenza viruses can induce some degree of protection against infection by a novel strain of influenza virus. Here, we assess the extent of protective immunity against infection with the 2009 influenza A (H1N1) pandemic influenza virus that is afforded by infection with a seasonal influenza A (H3N2) virus in mice. Mice that experienced a primary A (H3N2) influenza virus infection displayed reduced weight loss after challenge infection and cleared the 2009 influenza A (H1N1) virus infection more rapidly. To elucidate the correlates of protection of this heterosubtypic immunity to pandemic H1N1 virus infection, adoptive transfer experiments were carried out by using selected post-infection lymphocyte populations. Virus-specific CD8+ T-cells in concert with CD4+ T-cells were responsible for the observed protection. These findings may not only provide an explanation for epidemiological differences in the incidence of severe pandemic H1N1 infections, they also indicate that the induction of cross-reactive virus-specific CD8+ and CD4+ T-cell responses may be a suitable approach for the development of universal influenza vaccines.

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Cytotoxic T Lymphocytes Established by Seasonal Human Influenza Cross-React against 2009 Pandemic H1N1 Influenza Virus

Cited by 138 publications

References 59 publications

Seasonal influenza infection and live vaccine prime for a response to the 2009 pandemic H1N1 vaccine

Seasonal influenza infection and live vaccine prime for a response to the 2009 pandemic H1N1 vaccine

Vaccination with NS1-truncated H3N2 swine influenza virus primes T cells and confers cross-protection against an H1N1 heterosubtypic challenge in pigs

Cross-protective immunity against influenza pH1N1 2009 viruses induced by seasonal influenza A (H3N2) virus is mediated by virus-specific T-cells

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