Impact of preexisting memory to seasonal <scp>A</scp>/<scp>H</scp>1<scp>N</scp>1 influenza virus on the immune response following vaccination against avian <scp>A</scp>/<scp>H</scp>5<scp>N</scp>1 virus

Buricchi, Francesca; Bardelli, Monia; Malzone, Carmine; Capecchi, Barbara; Nicolay, Uwe; Fragapane, Elena; Castellino, Flora; Giudice, Giuseppe Del; Galli, Grazia; Finco, Oretta

doi:10.1002/eji.201242563

Cited by 13 publications

(9 citation statements)

References 27 publications

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“…1b). The moderate frequency of H5-specific memory B cells in subjects who were not exposed to H5N1 viruses or vaccines is likely a consequence of prior seasonal influenza vaccination and/or infection (18,19). Notably, at this time point there was no significant difference in the frequencies of H5-specific memory B cells between the H5N1 pLAIVprimed and unprimed or between the H5N1 pLAIV-primed and H7N3 pLAIV-primed subjects (P Ͼ 0.05, separate Mann-Whitney U tests) ( Fig.…”

Section: Resultsmentioning

confidence: 99%

Intranasal Live Influenza Vaccine Priming Elicits Localized B Cell Responses in Mediastinal Lymph Nodes

Jegaskanda

Mason

Andrews

et al. 2018

J Virol

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Pandemic live attenuated influenza vaccines (pLAIV) prime subjects for a robust neutralizing antibody response upon subsequent administration of a pandemic inactivated subunit vaccine (pISV). However, a difference was not detected in H5-specific memory B cells in the peripheral blood between pLAIV-primed and unprimed subjects prior to pISV boost. To investigate the mechanism underlying pLAIV priming, we vaccinated groups of 12 African green monkeys (AGMs) with H5N1 pISV or pLAIV alone or H5N1 pLAIV followed by pISV and examined immunity systemically and in local draining lymph nodes (LN). The AGM model recapitulated the serologic observations from clinical studies. Interestingly, H5N1 pLAIV induced robust germinal center B cell responses in the mediastinal LN (MLN). Subsequent boosting with H5N1 pISV drove increases in H5-specific B cells in the axillary LN, spleen, and circulation in H5N1 pLAIV-primed animals. Thus, H5N1 pLAIV primes localized B cell responses in the MLN that are recalled systemically following pISV boost. These data provide mechanistic insights for the generation of robust humoral responses via prime-boost vaccination. We have previously shown that pandemic live attenuated influenza vaccines (pLAIV) prime for a rapid and robust antibody response on subsequent administration of inactivated subunit vaccine (pISV). This is observed even in individuals who had undetectable antibody (Ab) responses following the initial vaccination. To define the mechanistic basis of pLAIV priming, we turned to a nonhuman primate model and performed a detailed analysis of B cell responses in systemic and local lymphoid tissues following prime-boost vaccination with pLAIV and pISV. We show that the nonhuman primate model recapitulates the serologic observations from clinical studies. Further, we found that pLAIVs induced robust germinal center B cell responses in the mediastinal lymph node. Subsequent boosting with pISV in pLAIV-primed animals resulted in detection of B cells in the axillary lymph nodes, spleen, and peripheral blood. We demonstrate that intranasally administered pLAIV elicits a highly localized germinal center B cell response in the mediastinal lymph node that is rapidly recalled following pISV boost into germinal center reactions at numerous distant immune sites.

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Section: Resultsmentioning

confidence: 99%

Intranasal Live Influenza Vaccine Priming Elicits Localized B Cell Responses in Mediastinal Lymph Nodes

Jegaskanda

Mason

Andrews

et al. 2018

J Virol

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“…Normally, the frequency of broadly neutralizing Abs that recognize highly conserved epitopes within the HA2 domain of the protein is very low and has been estimated to occur in only one in 100,000 HA-specific plasma cells (Corti et al, 2011). However, several studies have shown that these types of antibodies can be induced following heterologous primeboost vaccination and by using vaccine adjuvants that broaden heterosubtypic Ab responses (Buricchi et al, 2013; Chiu et al, 2013; Li et al, 2013). Thus, to enrich for cross-reactive Abs, mice were immunized with rHA isolated from 2 Group 1 HA viruses, VN1203 and CA07 virus, in the presence of the TLR4 adjuvant GLA-SE, which increases antibody repertoire diversity and enhances protection against heterosubtypic strains of H5N1 virus in mice and ferrets (Clegg et al, 2014; Clegg et al, 2012; Wiley et al, 2011).…”

Section: Resultsmentioning

confidence: 99%

Selection of therapeutic H5N1 monoclonal antibodies following IgVH repertoire analysis in mice

et al. 2016

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The rapid rate of influenza virus mutation drives the emergence of new strains that inflict serious seasonal epidemics and less frequent, but more deadly, pandemics. While vaccination provides the best protection against influenza, its utility is often diminished by the unpredictability of new pathogenic strains. Consequently, efforts are underway to identify new antiviral drugs and monoclonal antibodies that can be used to treat recently infected individuals and prevent disease in vulnerable populations. Next Generation Sequencing (NGS) and the analysis of antibody gene repertoires is a valuable tool for Ab discovery. Here, we describe a technology platform for isolating therapeutic monoclonal antibodies (MAbs) by analyzing the IgVH repertoires of mice immunized with recombinant H5N1 hemagglutinin (rH5). As an initial proof of concept, 35 IgVH genes selected using a CDRH3 search algorithm, co-expressed in a murine IgG2a expression vector with a panel of germline murine kappa genes, and culture supernatants screened for antigen binding. Seventeen of the 35 IgVH MAbs (49%) bound rH5VN1203 in preliminary screens and 8 of 9 purified MAbs inhibited 3 heterosubtypic strains of H5N1 virus when assayed by HI, and 2 MAbs demonstrated prophylactic and therapeutic activity in virus-challenged mice. This is the first example in which an NGS discovery platform has been used to isolate anti-influenza MAbs with relevant therapeutic activity.

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“…One can hypothesize that previous exposure to other subtypes may have offered protection against H5N1 [32].…”

Section: Discussionmentioning

confidence: 99%

Populations at Risk for Severe or Complicated Avian Influenza H5N1: A Systematic Review and Meta-Analysis

et al. 2014

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BackgroundLittle is known about risk factors for severe outcomes in patients infected with H5N1 and no systematic review has been conducted. Understanding risk factors is an important step for prioritizing prophylaxis or treatment in the event of a pandemic.ObjectivesTo systematically evaluate risk factors for severe outcomes in patients with avian influenza H5N1 infection.Data sourcesMEDLINE, EMBASE, CINAHL, GlobalHealth, and CENTRAL through March 2011Eligibility criteria for selecting studiesObservational studies of any design published in English, French, Spanish, German or Korean that reported on risk factor-outcome combinations of interest in participants with confirmed H5N1 infections. Outcomes considered included death, ventilator support, hospital and ICU admission, pneumonia, and composite outcomes.Study appraisalRisk of bias was assessed using the Newcastle-Ottawa scale (NOS).ResultsWe identified 20 studies reporting on 999 patients infected with H5N1. The majority of studies (n = 14, 70%) were at intermediate risk of bias, i.e. 4–6 points on the NOS. Females were at increased risk of death (OR 1.75, 95% CI 1.27–2.44), while young age, in particular <5 years of age (OR 0.44, 95% CI 0.25–0.79 for death), was protective. Data on traditional risk factors was scarce and requires further studies. Another major limitation in the published literature was lack of adjustment for confounders.InterpretationFemales were at increased risk for complications following H5N1 infection while young age protected against severe outcomes. Research on traditional risk factors was limited and is required.

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Impact of preexisting memory to seasonal A/H1N1 influenza virus on the immune response following vaccination against avian A/H5N1 virus

Cited by 13 publications

References 27 publications

Intranasal Live Influenza Vaccine Priming Elicits Localized B Cell Responses in Mediastinal Lymph Nodes

Intranasal Live Influenza Vaccine Priming Elicits Localized B Cell Responses in Mediastinal Lymph Nodes

Selection of therapeutic H5N1 monoclonal antibodies following IgVH repertoire analysis in mice

Populations at Risk for Severe or Complicated Avian Influenza H5N1: A Systematic Review and Meta-Analysis

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