How to assess the effectiveness of nasal influenza vaccines? Role and measurement of sIgA in mucosal secretions

Gianchecchi, Elena; Manenti, Alessandro; Kistner, Otfried; Trombetta, Claudia Maria; Manini, Ilaria; Montomoli, Emanuele

doi:10.1111/irv.12664

Cited by 35 publications

(31 citation statements)

References 85 publications

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“…Previous studies have shown that serum antibody levels are a poor measure of LAIV vaccine efficacy ( 50 ). In contrast, nasal mucosal secretory IgA, the predominant immunoglobulin produced in response to infection of the nasal mucosa, has been shown to be a much better indicator of LAIV-induced antibody responses (reviewed in Reference 45 ). We developed an anti–LAIV-IgA ELISA to determine the effects of cigarette smoking and e-cigarette use on antibody production and found that LAIV-specific IgA levels increased as expected in nonsmokers after LAIV inoculation but did not increase in e-cigarette users and cigarette smokers ( Figure 3B ).…”

Section: Resultsmentioning

confidence: 99%

“…Considering that e-cigarette use is prevalent among teenagers who are recommended for complete immunization schedules, understanding whether and how vaping could modify vaccination-conferred immunity is an unexplored field. Secretory IgA is the principal antibody isotype present in nasal secretions ( 45 ) and neutralizes pathogens, like influenza, at the site of infection before they attach, enter, and replicate in the host cell ( 45 ). Although conventional intramuscularly administered influenza vaccines generate a serum IgG-antibody response, protection conferred by LAIV vaccination is believed to be derived by its ability to generate a robust and sustained nasal mucosal IgA response ( 51 ).…”

Section: Discussionmentioning

confidence: 99%

“…Levels of influenza-specific IgA in the NLF were measured using a direct-sandwich ELISA ( see data supplement). Virus-specific IgA levels were determined against the IgA standard curve and normalized to total IgA levels ( 45 ). After normalization, the change in the antibody level was determined by using the relative percentage of the baseline level, in which the virus-specific antibody concentration post-LAIV inoculation was divided by pre-LAIV inoculation levels and multiplied by 100.…”

Section: Methodsmentioning

confidence: 99%

See 2 more Smart Citations

Electronic-Cigarette Use Alters Nasal Mucosal Immune Response to Live-attenuated Influenza Virus. A Clinical Trial

Rebuli

Glista-Baker

Hoffman³

et al. 2021

Am J Respir Cell Mol Biol

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

See 1 more Smart Citation

Electronic-Cigarette Use Alters Nasal Mucosal Immune Response to Live-attenuated Influenza Virus. A Clinical Trial

Rebuli

Glista-Baker

Hoffman³

et al. 2021

Am J Respir Cell Mol Biol

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“…SIgA antibodies have neutralization potential pathogens at the entrance site before they can attach to epithelial cells and overcome the epithelial surface. Considerable levels of Influenza virus specific SIgA was secreted in saliva, suggesting that saliva works as humoral immunity against influenza virus [ 20 , 21 ]. The development of mucosal vaccines that aim to induce influenza virus-specific IgA has been working on.…”

Section: The Influence Of Oral Health On Influenza Virus Infectionmentioning

confidence: 99%

The Impact of Oral Health on Respiratory Viral Infection

Tada

Senpuku

2021

Dentistry Journal

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Influenza virus and severe acute respiratory syndrome coronavirus (SARS-CoV-2) have caused respiratory diseases worldwide. Coronavirus disease 2019 (COVID-19) is now a global health concern requiring emergent measures. These viruses enter the human body through the oral cavity and infect respiratory cells. Since the oral cavity has a complex microbiota, influence of oral bacteria on respiratory virus infection is considered. Saliva has immune molecules which work as the front line in the biophylactic mechanism and has considerable influence on the incidence and progression of respiratory viral infection. Salivary scavenger molecules, such as gp340 and sialic acid, have been reported to exert anti-influenza virus activity. Salivary secretory immunoglobulin A (SIgA) has potential to acquire immunity against these viruses. Biological features of the oral cavity are thought to affect viral infection in respiratory organs in various ways. In this review, we reviewed the literature addressing the impact of oral conditions on respiratory infectious diseases caused by viruses.

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“…74 In mucosae, technical difficulties in obtaining samples also exist, although standardized methods in our laboratory and by others are optimal. 3,4,75,76 Immunogenicity-the ability of an immunogen to elicit high titers of Abs and T cell proliferation or cytokine secretion-is just the first step on the long way to obtain an efficacious vaccine. 77 One side of the problem is that we still lack enough understanding of the types of immune responses that protect the host from specific pathogens.…”

Section: Correlates Of Protection Against Mucosal Pathogens Are Not Ementioning

confidence: 99%

Induction of mucosal immunity against pathogens by using recombinant baculoviral vectors: Mechanisms, advantages, and limitations

Fragoso-Saavedra

Vega-Lopez

2020

Journal of Leukocyte Biology

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Over 90% of pathogens of medical importance invade the organism through mucosal surfaces, which makes it urgent to develop safe and effective mucosal vaccines and mucosal immunization protocols. Besides, parenteral immunization does not provide adequate protective immunity in mucosal surfaces. Effective mucosal vaccination could protect local and systemic compartments and favor herd immunity. Although various mucosal adjuvants and Ag‐delivery systems have been developed, none has filled the gap to control diseases caused by complex mucosal pathogens. Among the strategies to counteract them, recombinant virions from the baculovirus Autographa californica multiple nucleopolyhedrovirus (rAcMNPV) are useful vectors, given their safety and efficacy to produce mucosal and systemic immunity in animal infection models. Here, we review the immunogenic properties of rAcMNPV virions from the perspectives of mucosal immunology and vaccinology. Some features, which are analyzed and extrapolated from studies with different particulate antigens, include size, shape, surface molecule organization, and danger signals, all needed to break the tolerogenic responses of the mucosal immune tissues. Also, we present a condensed discussion on the immunity provided by rAcMNPV virions against influenza virus and human papillomavirus in animal models. Through the text, we highlight the advantages and limitations of this experimental immunization platform.

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How to assess the effectiveness of nasal influenza vaccines? Role and measurement of sIgA in mucosal secretions

Cited by 35 publications

References 85 publications

Electronic-Cigarette Use Alters Nasal Mucosal Immune Response to Live-attenuated Influenza Virus. A Clinical Trial

Electronic-Cigarette Use Alters Nasal Mucosal Immune Response to Live-attenuated Influenza Virus. A Clinical Trial

The Impact of Oral Health on Respiratory Viral Infection

Induction of mucosal immunity against pathogens by using recombinant baculoviral vectors: Mechanisms, advantages, and limitations

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