Development of an influenza virus protein microarray to measure the humoral response to influenza virus infection in mallards

Meade, Philip; Latorre‐Margalef, Neus; Stallknecht, David E.; Krammer, Florian

doi:10.1038/emi.2017.98

Cited by 21 publications

(25 citation statements)

References 40 publications

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“…This method was chosen because it is more quantitative than assaying one serum dilution only. We have also shown in the past (13) and here that the method correlates well with ELISA results, can detect antibodies with high specificity, and can detect broadly neutralizing antibodies that bind to fragile and conformational epitopes (Fig. S2).…”

Section: Methodssupporting

confidence: 71%

“…However, performing individual ELISAs against recombinant HAs of many different virus strains and subtypes is tedious and timeconsuming and can be sample intensive. Recently, we therefore developed influenza virus protein microarrays (IVPMs) (13). For this technology, we print a library of recombinant HA proteins, including all HA subtypes, on microarrays which are then probed with serial dilutions of serum (see Fig.…”

mentioning

confidence: 99%

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Influenza Virus Infection Induces a Narrow Antibody Response in Children but a Broad Recall Response in Adults

Meade

Kuan

Strohmeier

et al. 2020

mBio

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In contrast to influenza virus vaccination, natural infection induces long-lived and relatively broad immune responses. However, many aspects of the antibody response to natural infection are not well understood. Here, we assessed the immune response after H1N1 influenza virus infection in children and adults in a Nicaraguan household transmission study using an influenza virus protein microarray (IVPM). This technology allows us to simultaneously measure IgG and IgA antibody responses to hemagglutinins of many different virus strains and subtypes quantitatively with a high throughput. We found that children under 6 years of age responded to natural infection with a relatively narrow response that targeted mostly the hemagglutinin of the strain that caused the infection. Adults, however, have a much broader response, including a boost in antibodies to many group 1 subtype hemagglutinins. Also, a strong recall response against historic H1 hemagglutinins that share the K133 epitope with the pandemic H1N1 virus was observed. Of note, some children, while responding narrowly within H1 and group 1 hemagglutinins, induced a boost to H3 and other group 2 hemagglutinins when infected with H1N1 when they had experienced an H3N2 infection earlier in life. This is an interesting phenomenon providing evidence for immune imprinting and a significant new insight which might be leveraged in future universal influenza virus vaccine strategies. Finally, preexisting immunity to pandemic H1 hemagglutinins was significantly associated with protection from infection in both children and adults. In adults, preexisting immunity to non-H1 group 1 hemagglutinins was also significantly associated with protection from infection. IMPORTANCE It is known since Thomas Francis, Jr. published his first paper on original antigenic sin in 1960 that the first infection(s) with influenza virus leaves a special immunological imprint which shapes immune responses to future infections with antigenically related influenza virus strains. Imprinting has been implicated in both protective effects as well as blunting of the immune response to vaccines. Despite the fact that this phenomenon was already described almost 60 years ago, we have very little detailed knowledge of the characteristics and breadth of the immune response to the first exposure(s) to influenza virus in life and how this compares to later exposure as adults. Here, we investigate these immune responses in detail using an influenza virus protein microarray. While our findings are mostly descriptive in nature and based on a small sample size, they provide a strong basis for future large-scale studies to better understand imprinting effects.

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Section: Methodssupporting

confidence: 71%

mentioning

confidence: 99%

Influenza Virus Infection Induces a Narrow Antibody Response in Children but a Broad Recall Response in Adults

Meade

Kuan

Strohmeier

et al. 2020

mBio

Self Cite

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“…14 Cross reactive CD4+ and CD8+ cells have also been identified as correlates of protection in human challenge and cohort studies. [4][5][6][7] Other immunological markers, including antibody effector functions as measured in antibody-dependent cellular cytotoxicity (ADCC) or antibody-dependent cell-mediated phagocytosis (ADCP) assays, 25-28 complement activation, mucosal antibody levels, entry inhibition titers as measured by pseudotype particle entry inhibition assays, 29 antibodies to the ectodomain of the matrix 2 ion channel (M2e), antibodies to matrix protein 1 (M1) and nucleoprotein (NP), 30 influenza virus protein arrays (IVPM), [31][32][33][34] and many others are currently being investigated to assess whether they correlate with protection. Importantly, systems immunology approaches are being used to identify new immunological markers that could then be tested for their potential to predict whether protective immunity was induced through vaccination.…”

Section: E Xis Ting and Novel Correl Ate S Of Protec Ti Onmentioning

confidence: 99%

“…Cell-based ELISA or flow cytometry 30 Influenza virus proteins Influenza virus protein arrays (IVPM) [31][32][33][34] Immune markers Systems immunology 35,36 validation.). Standardization of sampling is also useful in this context.…”

Section: Viral Entry Inhibition Antibodiesmentioning

confidence: 99%

Meeting report and review: Immunological assays and correlates of protection for next‐generation influenza vaccines

Krammer

Weir

Engelhardt

et al. 2019

Influenza Resp Viruses

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Background This report summarizes the discussions and conclusions from the “Immunological Assays and Correlates of Protection for Next‐Generation Influenza Vaccines” meeting which took place in Siena, Italy, from March 31, 2019, to April 2, 2019. Conclusions Furthermore, we review current correlates of protection against influenza virus infection and disease and their usefulness for the development of next generation broadly protective and universal influenza virus vaccines.

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“…Building on extensive previous work by multiple contributors in the field 15,16,17,18,19 , an influenza protein microarray was recently developed that contains over 250 purified hemagglutinin (HA) antigenic variants with representation of all 18 subtypes 12,20 . Using this methodology, a natural influenza infection was demonstrated to generate broadly reactive IgG and IgA antibodies against phylogenetically related HA subtypes, while an intramuscular influenza vaccination generated only subtype-specific IgG antibodies 21 .…”

Section: Introductionmentioning

confidence: 99%

Use of an Influenza Antigen Microarray to Measure the Breadth of Serum Antibodies Across Virus Subtypes

Khan

Jain

Taghavian

et al. 2019

JoVE

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The influenza virus remains a significant cause of mortality worldwide due to the limited effectiveness of currently available vaccines. A key challenge to the development of universal influenza vaccines is high antigenic diversity resulting from antigenic drift. Overcoming this challenge requires novel research tools to measure the breadth of serum antibodies directed against many virus strains across different antigenic subtypes. Here, we present a protocol for analyzing the breadth of serum antibodies against diverse influenza virus strains using a protein microarray of influenza antigens. This influenza antigen microarray is constructed by printing purified hemagglutinin and neuraminidase antigens onto a nitrocellulose-coated membrane using a microarray printer. Human sera are incubated on the microarray to bind antibodies against the influenza antigens. Quantumdot-conjugated secondary antibodies are used to simultaneously detect IgG and IgA antibodies binding to each antigen on the microarray. Quantitative antibody binding is measured as fluorescence intensity using a portable imager. Representative results are shown to demonstrate assay reproducibility in measuring subtype-specific and cross-reactive influenza antibodies in human sera. Compared to traditional methods such as ELISA, the influenza antigen microarray provides a high throughput multiplexed approach capable of testing hundreds of sera for multiple antibody isotypes against hundreds of antigens in a short time frame, and thus has applications in serosurveillance and vaccine development. A limitation is the inability to distinguish binding antibodies from neutralizing antibodies. Video Link The video component of this article can be found at https://www.jove.com/video/59973/ Protein microarrays, potentially consisting of up to thousands of antigens printed onto nitrocellulose-coated slides as shown in Figure 1, can fill this need 12. These microarrays can be produced and probed in a high throughput manner while consuming small quantities of clinical specimen

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Development of an influenza virus protein microarray to measure the humoral response to influenza virus infection in mallards

Cited by 21 publications

References 40 publications

Influenza Virus Infection Induces a Narrow Antibody Response in Children but a Broad Recall Response in Adults

Influenza Virus Infection Induces a Narrow Antibody Response in Children but a Broad Recall Response in Adults

Meeting report and review: Immunological assays and correlates of protection for next‐generation influenza vaccines

Use of an Influenza Antigen Microarray to Measure the Breadth of Serum Antibodies Across Virus Subtypes

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