Your search keyword '"McMahon, Meagan"' showing total 10 results

1. Assessment of a quadrivalent nucleoside-modified mRNA vaccine that protects against group 2 influenza viruses.

Author

McMahon, Meagan, O’Dell, George, Tan, Jessica, Sárközy, András, Vadovics, Máté, Carreño, Juan Manuel, Puente-Massaguer, Eduard, Muramatsu, Hiromi, Bajusz, Csaba, Rijnink, Willemijn, Beattie, Mitchell, Tam, Ying K., Roubidoux, Ericka Kirkpatrick, Francisco, Isabel, Strohmeier, Shirin, Kanekiyo, Masaru, Graham, Barney S., Krammer, Florian, and Pardi, Norbert

Subjects

*INFLUENZA viruses, *INFLUENZA A virus, *INFLUENZA A virus, H1N1 subtype, *COMBINED vaccines, *GROUP psychotherapy, *INFLUENZA vaccines, *COST effectiveness

Abstract

Combined vaccine formulations targeting not only hemagglutinin but also other influenza virus antigens could form the basis for a universal influenza virus vaccine that has the potential to elicit long-lasting, broadly cross-reactive immune responses. Lipid nanoparticle (LNP)-encapsulated messenger RNA (mRNA) vaccines can be utilized to efficiently target multiple antigens with a single vaccine. Here, we assessed the immunogenicity and protective efficacy of nucleoside-modified mRNA-LNP vaccines that contain four influenza A group 2 virus antigens (hemagglutinin stalk, neuraminidase, matrix protein 2, and nucleoprotein) in mice. We found that all vaccine components induced antigen-specific cellular and humoral immune responses after administration of a single dose. While the monovalent formulations were not exclusively protective, the combined quadrivalent formulation protected mice from all challenge viruses, including a relevant H1N1 influenza virus group 1 strain, with minimal weight loss. Importantly, the combined vaccine protected from morbidity at a dose of 125 ng per antigen after a single vaccination in mice. With these findings, we confidently conclude that the nucleoside-modified mRNA-LNP platform can be used to elicit protection against a large panel of influenza viruses. [ABSTRACT FROM AUTHOR]

Published

2022

2. Development of a pentavalent broadly protective nucleoside-modified mRNA vaccine against influenza B viruses.

Author

Pardi, Norbert, Carreño, Juan Manuel, O'Dell, George, Tan, Jessica, Bajusz, Csaba, Muramatsu, Hiromi, Rijnink, Willemijn, Strohmeier, Shirin, Loganathan, Madhumathi, Bielak, Dominika, Sung, Molly M. H., Tam, Ying K., Krammer, Florian, and McMahon, Meagan

Subjects

INFLUENZA, INFLUENZA viruses, INFLUENZA vaccines, INFLUENZA B virus, VACCINE effectiveness, MESSENGER RNA, CAPACITY building

Abstract

Messenger RNA (mRNA) vaccines represent a new, effective vaccine platform with high capacity for rapid development. Generation of a universal influenza virus vaccine with the potential to elicit long-lasting, broadly cross-reactive immune responses is a necessity for reducing influenza-associated morbidity and mortality. Here we focus on the development of a universal influenza B virus vaccine based on the lipid nanoparticle-encapsulated nucleoside-modified mRNA (mRNA-LNP) platform. We evaluate vaccine candidates based on different target antigens that afford protection against challenge with ancestral and recent influenza B viruses from both antigenic lineages. A pentavalent vaccine combining all tested antigens protects mice from morbidity at a very low dose of 50 ng per antigen after a single vaccination. These findings support the further advancement of nucleoside-modified mRNA-LNPs expressing multiple conserved antigens as universal influenza virus vaccine candidates. The public health concern caused by influenza B virus is often overlooked, yet represents a significant global burden. Here, the authors evaluate the cellular and humoral immune responses of multivalent vaccine candidates, based on the lipid nanoparticle-encapsulated nucleoside-modified mRNA platform, and demonstrate protection of mice from challenge with a broad panel of influenza B viruses. [ABSTRACT FROM AUTHOR]

Published

2022

3. Correctly folded - but not necessarily functional - influenza virus neuraminidase is required to induce protective antibody responses in mice.

Author

McMahon, Meagan, Strohmeier, Shirin, Rajendran, Madhusudan, Capuano, Christina, Ellebedy, Ali H., Wilson, Patrick C., and Krammer, Florian

Subjects

*INFLUENZA A virus, *NEURAMINIDASE, *ANTIBODY formation, *INFLUENZA B virus, *INFLUENZA vaccines, *SEASONAL influenza

Abstract

The influenza virus neuraminidase (NA) plays an integral role in the influenza virus life cycle through the release of virions from infected cells. NA-specific antibodies can impede virus replication by binding to the NA and blocking its enzymatic activity, providing significant protection from influenza-associated morbidity and mortality. NA included in current seasonal influenza virus vaccines exhibits low immunogenicity, potentially caused by compromised antigenic integrity during vaccine production. To determine how certain types of "stress" could influence the antigenicity of NA we performed a series of in vitro experiments where we treated NA with formalin, EDTA or heat and measured the impact of these treatments on NA enzymatic activity and structural integrity. We found that increasing concentrations of formalin or EDTA and increasing temperature abolished the enzymatic activity of both H1N1, H3N2, and influenza B purified viruses and recombinant NA proteins. However, formalin and EDTA treatment did not drastically affect conformational epitopes found on the NA, whereas heat treatment abolished conformational epitopes. We next performed a vaccination experiment, where mice were vaccinated with recombinant N2 NA treated with 0.3% formalin or 0.125 M EDTA (which both inactivated NA activity) were protected from virus challenge while animals vaccinated with heat treated NA were not. We next tested the protective effect of monomeric (no enzymatic activity) versus tetrameric (highly active) N1 NA. Again, only the tetrameric form protected mice from challenge while the monomeric form did not. Together, our data demonstrate that enzymatically active NA is not required to induce protective antibody responses as a vaccine, however a correctly folded NA is essential. [ABSTRACT FROM AUTHOR]

Published

2020

4. Vaccination with viral vectors expressing NP, M1 and chimeric hemagglutinin induces broad protection against influenza virus challenge in mice.

Author

Asthagiri Arunkumar, Guha, McMahon, Meagan, Pavot, Vincent, Aramouni, Mario, Ioannou, Andriani, Lambe, Teresa, Gilbert, Sarah, and Krammer, Florian

Subjects

*HEMAGGLUTININ, *INFLUENZA A virus, *INFLUENZA vaccines, *INFLUENZA A virus, H3N2 subtype, *VACCINATION, *VIRUS diseases, *PANDEMICS

Abstract

Seasonal influenza virus infections cause significant morbidity and mortality every year. Annual influenza virus vaccines are effective but only when well matched with circulating strains. Therefore, there is an urgent need for better vaccines that induce broad protection against drifted seasonal and emerging pandemic influenza viruses. One approach to design such vaccines is based on targeting conserved regions of the influenza virus hemagglutinin. Sequential vaccination with chimeric hemagglutinin constructs can refocus antibody responses towards the conserved immunosubdominant stalk domain of the hemagglutinin, rather than the variable immunodominant head. A complementary approach for a universal influenza A virus vaccine is to induce T-cell responses to conserved internal influenza virus antigens. For this purpose, replication deficient recombinant viral vectors based on Chimpanzee Adenovirus Oxford 1 and Modified Vaccinia Ankara virus are used to express the viral nucleoprotein and the matrix protein 1. In this study, we combined these two strategies and evaluated the efficacy of viral vectors expressing both chimeric hemagglutinin and nucleoprotein plus matrix protein 1 in a mouse model against challenge with group 2 influenza viruses including H3N2, H7N9 and H10N8. We found that vectored vaccines expressing both sets of antigens provided enhanced protection against H3N2 virus challenge when compared to vaccination with viral vectors expressing only one set of antigens. Vaccine induced antibody responses against divergent group 2 hemagglutinins, nucleoprotein and matrix protein 1 as well as robust T-cell responses to the nucleoprotein and matrix protein 1 were detected. Of note, it was observed that while antibodies to the H3 stalk were already boosted to high levels after two vaccinations with chimeric hemagglutinins (cHAs), three exposures were required to induce strong reactivity across subtypes. Overall, these results show that a combinations of different universal influenza virus vaccine strategies can induce broad antibody and T-cell responses and can provide increased protection against influenza. [ABSTRACT FROM AUTHOR]

Published

2019

5. The Human Antibody Response to the Influenza Virus Neuraminidase Following Infection or Vaccination.

Author

Rajendran, Madhusudan, Krammer, Florian, and McMahon, Meagan

Subjects

ANTIBODY formation, INFLUENZA A virus, NEURAMINIDASE, INFLUENZA viruses, INFLUENZA vaccines

Abstract

The influenza virus neuraminidase (NA) is primarily involved in the release of progeny viruses from infected cells—a critical role for virus replication. Compared to the immuno-dominant hemagglutinin, there are fewer NA subtypes, and NA experiences a slower rate of antigenic drift and reduced immune selection pressure. Furthermore, NA inhibiting antibodies prevent viral egress, thus preventing viral spread. Anti-NA immunity can lessen disease severity, reduce viral shedding, and decrease viral lung titers in humans and various animal models. As a result, there has been a concerted effort to investigate the possibilities of incorporating immunogenic forms of NA as a vaccine antigen in future vaccine formulations. In this review, we discuss NA-based immunity and describe several human NA-specific monoclonal antibodies (mAbs) that have a broad range of protection. We also review vaccine platforms that are investigating NA antigens in pre-clinical models and their potential use for next-generation influenza virus vaccines. The evidence presented here supports the inclusion of immunogenic NA in future influenza virus vaccines. [ABSTRACT FROM AUTHOR]

Published

2021

6. Novel Epitopes of the Influenza Virus N1 Neuraminidase Targeted by Human Monoclonal Antibodies.

Author

Roubidoux, Ericka Kirkpatrick, Sano, Kaori, McMahon, Meagan, Manuel Carreño, Juan, Capuano, Christina, Kaijun Jiang, Simon, Viviana, van Bakel, Harm, Wilson, Patrick, and Krammer, Florian

Subjects

*NEURAMINIDASE, *MONOCLONAL antibodies, *INFLUENZA A virus, *INFLUENZA viruses, *INFLUENZA vaccines, *EPITOPES, *PROTEIN domains

Abstract

Influenza virus neuraminidase (NA)-targeting antibodies are an independent correlate of protection against influenza. Antibodies against the NA act by blocking enzymatic activity, preventing virus release and transmission. As we advance the development of improved influenza virus vaccines that incorporate standard amounts of NA antigen, it is important to identify the antigenic targets of human monoclonal antibodies (mAbs). Here, we describe escape mutants generated by serial passage of A/Netherlands/602/2009 (H1N1)pdm09 in the presence of human anti-N1 mAbs. We observed escape mutations on the head domain of the N1 protein around the enzymatic site (S364N, N369T, and R430Q) and also detected escape mutations located on the sides and bottom of the NA (N88D, N270D, and Q313K/R). This work increases our understanding of how human antibody responses target the N1 protein. [ABSTRACT FROM AUTHOR]

Published

2022

7. Female-biased effects of aging on a chimeric hemagglutinin stalk-based universal influenza virus vaccine in mice.

Author

Dhakal, Santosh, Deshpande, Sharvari, McMahon, Meagan, Strohmeier, Shirin, Krammer, Florian, and Klein, Sabra L.

Subjects

*INFLUENZA, *INFLUENZA vaccines, *HEMAGGLUTININ, *ANTIBODY-dependent cell cytotoxicity, *SEX (Biology), *YOUNG adults, *INFLUENZA A virus, H1N1 subtype, *MICE

Abstract

• Antibody responses and protection to a cHA-based universal influenza virus vaccine declines with advanced age. • Age-associated decline in antibody responses and protection is more prominent in females than males. • Serum from vaccinated adult mice is not sufficient to protect naïve aged, sex-matched mice. • Age and sex should be considered in preclinical and clinical studies with universal influenza virus vaccines. To determine if biological sex and age intersect to affect universal influenza vaccine-induced immunity, adult and aged male and female C57BL/6 mice were sequentially immunized with a chimeric-hemagglutinin (cHA) stalk-based H1 vaccine. Adult mice developed greater quantity and quality of H1-stalk antibodies, that were more cross-reactive with other group 1, but not group 2, influenza viruses, than aged mice. The vaccine did not induce neutralizing or hemagglutination inhibition antibodies, but rather antibody-dependent cellular cytotoxicity, which was greater in adult than aged mice. Vaccinated adult mice were better protected than aged mice after challenge with 2009 H1N1 virus, experiencing less morbidity and having lower pulmonary virus titers. The age-associated decline in immunity and protection was consistently greater among females than males, with the reduction in immunity and protection for aged as compared with adult females often being the sole comparison driving the overall age-associated significant differences. The age-associated reduction in stalk-based immunity in females was not, however, associated with changes in estradiol. To determine if the better antibodies in adults could be utilized to protect aged mice, serum was passively transferred from vaccinated adult mice into naïve sex-matched aged mice. Even with transferred serum from young adult mice, aged females still suffered greater morbidity than aged males. These data suggest there are sex-dependent effects of aging on cHA-based universal influenza virus vaccine-induced immunity that cannot be reversed through transfer of serum from young animals. The lack of consideration of sex-specific effects of aging on immunity could hinder efforts toward universal vaccines. [ABSTRACT FROM AUTHOR]

Published

2022

8. Characterization of Novel Cross-Reactive Influenza B Virus Hemagglutinin Head Specific Antibodies That Lack Hemagglutination Inhibition Activity.

Author

Kirkpatrick, Ericka, Henry, Carole, McMahon, Meagan, Kaijun Jiang, Strohmeier, Shirin, van Bakel, Harm, Wilson, Patrick C., and Krammer, Florian

Subjects

*INFLUENZA B virus, *MONOCLONAL antibodies, *OLDER people, *HEMAGGLUTININ, *FLU vaccine efficacy, *INFLUENZA vaccines, *VIRAL antibodies

Abstract

Humoral immune responses to influenza virus vaccines in elderly individuals are poorly adapted toward new antigenically drifted influenza virus strains. Instead, older individuals respond in an original antigenic sin fashion and produce much more cross-reactive but less potent antibodies. Here, we investigated four influenza B virus hemagglutinin (HA) head specific, hemagglutination inhibitioninactive monoclonal antibodies (MAbs) from elderly individuals. We found that they were broadly reactive within the B/Victoria/2/1987-like lineage, and two were highly cross-reactive with B/Yamagata/16/1988-like lineage viruses. The MAbs were found to be neutralizing, to utilize Fc effector functions, and to be protective against lethal viral challenge in a mouse model. In order to identify residues on the influenza B virus hemagglutinin interacting with the MAbs, we generated escape mutant viruses. Interestingly, escape from these MAbs led to numerous HA mutations within the head domain, including in the defined antigenic sites. We observed that each individual escape mutant virus was able to avoid neutralization by its respective MAb along with other MAbs in the panel, although in many cases binding activity was maintained. Point mutant viruses indicated that K90 is critical for the neutralization of two MAbs, while escape from the other two MAbs required a combination of mutations in the hemagglutinin. Three of four escape mutant viruses had increased lethality in the DBA2/J mouse model. Our work indicates that these cross-reactive antibodies have the potential to cause antigenic drift in the viral population by driving mutations that increase virus fitness. However, binding activity and cross-neutralization were maintained by a majority of antibodies in the panel, suggesting that this drift may not lead to escape from antibody-mediated protection. [ABSTRACT FROM AUTHOR]

Published

2020

9. Broadly protective human antibodies that target the active site of influenza virus neuraminidase.

Author

Stadlbauer, Daniel, Xueyong Zhu, McMahon, Meagan, Turner, Jackson S., Wohlbold, Teddy J., Schmitz, Aaron J., Strohmeier, Shirin, Wenli Yu, Nachbagauer, Raffael, Mudd, Philip A., Wilson, Ian A., Ellebedy, Ali H., and Krammer, Florian

Subjects

*INFLUENZA vaccines, *IMMUNOGLOBULINS, *NEURAMINIDASE, *HEMAGGLUTININ, *MONOCLONAL antibodies, *MEMBRANE glycoproteins

Abstract

Better vaccines against influenza virus are urgently needed to provide broader protection against diverse strains, subtypes, and types. Such efforts are assisted by the identification of novel broadly neutralizing epitopes targeted by protective antibodies. Influenza vaccine development has largely focused on the hemagglutinin, but the other major surface antigen, the neuraminidase, has reemerged as a potential target for universal vaccines. We describe three human monoclonal antibodies isolated from an H3N2-infected donor that bind with exceptional breadth to multiple different influenza A and B virus neuraminidases. These antibodies neutralize the virus, mediate effector functions, are broadly protective in vivo, and inhibit neuraminidase activity by directly binding to the active site. Structural and functional characterization of these antibodies will inform the development of neuraminidase-based universal vaccines against influenza virus. [ABSTRACT FROM AUTHOR]

Published

2019

10. Characterization of non-neutralizing human monoclonal antibodies that target the M1 and NP of influenza A viruses.

Author

Rijnink, Willemijn Frederique, Stadlbauer, Daniel, Puente-Massaguer, Eduard, Okba, Nisreen M. A., Roubidoux, Ericka Kirkpatrick, Strohmeier, Shirin, Mudd, Philip A., Schmitz, Aaron, Ellebedy, Ali, McMahon, Meagan, and Krammer, Florian

Subjects

*MONOCLONAL antibodies, *INFLUENZA viruses, *EXTRACELLULAR matrix proteins, *INFLUENZA vaccines, *WEIGHT loss, *SEASONAL influenza

Abstract

Improved broad-spectrum influenza virus vaccines are desperately needed to provide protection against both drifted seasonal and emerging pandemic influenza A viruses (IAVs). Antibody-based protection from influenza A virus-induced morbidity and mortality is traditionally associated with neutralizing antibodies. As such, vaccine efforts have solely focused on the hemagglutinin (HA) as a vaccine target; however, the HA is mutation prone resulting in the need for annual vaccine reformulation. Broad-spectrum vaccines could be achieved through non-neutralizing antibodies that target conserved influenza virus antigens. Here, we describe six human monoclonal antibodies (mAbs) isolated from two H3N2-infected donors that showed robust binding against the conserved internal nucleoprotein (NP) or matrix protein 1 (M1) of IAV strains. Despite the capacity for potent antigen binding, substantial morbidity was observed in mice prophylactically treated with these mAbs and then challenged with A/Netherlands/602/2009 (H1N1) or A/Switzerland/9715293/2013 (H3N2) viruses. While our findings need to be confirmed with a larger number of mAbs and with polyclonal serum, these findings suggest that human NP and M1 antibodies that are elicited following IAV infection/vaccination do not protect from substantial weight loss in the mouse model and imply that protection afforded targeting these antigens following vaccination/infection is most likely the result of cellular-based immunity. [ABSTRACT FROM AUTHOR]

Published

2023