Comparative Efficacy of Monoclonal Antibodies That Bind to Different Epitopes of the 2009 Pandemic H1N1 Influenza Virus Neuraminidase

Jiang, Lianlian; Fantoni, Giovanna; Couzens, Laura; Gao, Jin; Plant, Ewan P.; Ye, Zhiping; Eichelberger, Maryna C.; Wan, Hongquan

doi:10.1128/jvi.01756-15

Cited by 50 publications

(61 citation statements)

References 39 publications

(62 reference statements)

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“…The NA protein is essential for release of virus particles from infected cells and decoy receptors (e.g., in mucus) and for preventing virion aggregation. The NA protein is also an important target of the immune response and antiviral drugs (1)(2)(3). The IAV NA protein appears, however, understudied compared to the HA protein.…”

mentioning

confidence: 99%

Substrate Binding by the Second Sialic Acid-Binding Site of Influenza A Virus N1 Neuraminidase Contributes to Enzymatic Activity

Dai

et al. 2018

J Virol

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The influenza A virus (IAV) neuraminidase (NA) protein plays an essential role in the release of virus particles from cells and decoy receptors. The NA enzymatic activity presumably needs to match the activity of the IAV hemagglutinin (HA) attachment protein and the host sialic acid (SIA) receptor repertoire. We analyzed the enzymatic activities of N1 NA proteins derived from avian (H5N1) and human (H1N1) IAVs and analyzed the role of the second SIA-binding site, located adjacent to the conserved catalytic site, therein. SIA contact residues in the second SIA-binding site of NA are highly conserved in avian, but not human, IAVs. All N1 proteins preferred cleaving α2,3- over α2,6-linked SIAs even when their corresponding HA proteins displayed a strict preference for α2,6-linked SIAs, indicating that the specificity of the NA protein does not need to fully match that of the corresponding HA protein. NA activity was affected by substitutions in the second SIA-binding site that are observed in avian and human IAVs, at least when multivalent rather than monovalent substrates were used. These mutations included both SIA contact residues and residues that do not directly interact with SIA in all three loops of the second SIA-binding site. Substrate binding via the second SIA-binding site enhanced the catalytic activity of N1. Mutation of the second SIA-binding site was also shown to affect virus replication Our results indicate an important role for the N1 second SIA-binding site in binding to and cleavage of multivalent substrates. Avian and human influenza A viruses (IAVs) preferentially bind α2,3- and α2,6-linked sialic acids (SIAs), respectively. A functional balance between the hemagglutinin (HA) attachment and neuraminidase (NA) proteins is thought to be important for host tropism. What this balance entails at the molecular level is, however, not well understood. We now show that N1 proteins of both avian and human viruses prefer cleaving avian- over human-type receptors although human viruses were relatively better in cleavage of the human-type receptors. In addition, we show that substitutions at different positions in the second SIA-binding site found in NA proteins of human IAVs have a profound effect on binding and cleavage of multivalent, but not monovalent, receptors and affect virus replication. Our results indicate that the HA-NA balance can be tuned via modification of substrate binding via this site and suggest an important role of the second SIA-binding site in host tropism.

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confidence: 99%

Substrate Binding by the Second Sialic Acid-Binding Site of Influenza A Virus N1 Neuraminidase Contributes to Enzymatic Activity

Dai

et al. 2018

J Virol

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“…These antibodies all bind to Cal09 NA and inhibit NA catalytic activity to varying degrees. HF5 and CD6 are strain-specific antibodies that each target distinct epitopes, and strongly inhibit NA activity as measured by ELLA [5]. Antibodies 1H5 and 4E9 recognize a similar epitope on the lateral surface of the NA head that is conserved across the N1 subtype, but these antibodies only weakly inhibit NA activity in ELLA assays [5].…”

Section: Anti-na Monoclonal Antibodies Neutralize a Na-binding-dependmentioning

confidence: 99%

“…NA also plays an important role in vivo by helping the virus penetrate mucus barriers to reach target cells [2,3]. Because only HA is needed for viral entry, anti-NA antibodies are not strongly neutralizing in infection assays where viruses are only allowed to undergo a single cycle of growth [4,5]. However, many studies have shown that anti-NA antibodies are associated with reduced disease severity in humans [6][7][8].…”

Section: Introductionmentioning

confidence: 99%

“…Here, we utilize the G147R NA in conjunction with a binding-deficient HA to develop a sensitive neutralization assay for anti-NA antibodies. Specifically, we test the susceptibility of this NAbinding-dependent virus to neutralization by four monoclonal antibodies targeting distinct epitopes of N1 NA [5], and find that some of these antibodies neutralize the NA-binding-dependent virus much better than they neutralize virus that can bind cells via HA. We then leverage this discovery to select an in vitro escape mutation to one of the antibodies, demonstrating the value of these viruses for antigenic mapping.…”

Section: Introductionmentioning

confidence: 99%

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Antibody neutralization of an influenza virus that uses neuraminidase for receptor binding

Gentles

Wan

Eichelberger

et al. 2020

Preprint

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Influenza virus infection elicits antibodies against the receptor-binding protein hemagglutinin (HA) and the receptor-cleaving protein neuraminidase (NA). Because HA is essential for viral entry, antibodies targeting HA often potently neutralize the virus in single-cycle infection assays. But antibodies against NA are not potently neutralizing in such assays, since NA is dispensable for single-cycle infection. Here we show that a modified influenza virus that depends on NA for receptor binding is much more sensitive than a virus with receptor-binding HA to neutralization by some anti-NA antibodies. Specifically, virus with a receptor-binding G147R N1 NA and a binding-deficient HA is completely neutralized in single-cycle infections by an antibody that binds near the NA active site. Infection is also substantially inhibited by antibodies that bind NA epitopes distant from the active site. Finally, we demonstrate that this modified virus can be used to efficiently select mutations in NA that escape antibody binding, a task that can be laborious with typical influenza viruses that are not well-neutralized by anti-NA antibodies. Thus, viruses dependent on NA for receptor binding allow for sensitive in vitro detection of antibodies binding near the catalytic site of NA and enable selection of viral escape mutants.

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“…Six of these mAbs are directed against various epitopes contained within the HA surface protein while one targets the matrix protein 2 (M2). In addition to the HA and M2, anti-neuraminidase (NA) mAb have also proven to be protective in the mouse model but, to our knowledge, have yet to enter clinical development (Doyle et al, 2013; Jiang et al, 2015; Shoji et al, 2011; Wan et al, 2013; Wohlbold et al, 2016; DiLillo et al, 2016). One potential concern regarding mAb as antivirals include the possibility that their use may drive the evolution of viral escape mutations which could be resistant not only to the mAb but to natural or vaccine-induced immunity.…”

Section: Introductionmentioning

confidence: 99%

An influenza A virus (H7N9) anti-neuraminidase monoclonal antibody protects mice from morbidity without interfering with the development of protective immunity to subsequent homologous challenge

et al. 2017

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The emergence of A(H7N9) virus strains with resistance to neuraminidase (NA) inhibitors highlights a critical need to discover new countermeasures for treatment of A(H7N9) virus-infected patients. We previously described an anti-NA mAb (3c10-3) that has prophylactic and therapeutic efficacy in mice lethally challenged with A(H7N9) virus when delivered intraperitoneally (i.p.). Here we show that intrananasal (i.n.) administration of 3c10-3 protects 100% of mice from mortality when treated 24 h post-challenge and further characterize the protective efficacy of 3c10-3 using a nonlethal A(H7N9) challenge model. Administration of 3c10-3 i.p. 24 h prior to challenge resulted in a significant decrease in viral lung titers and deep sequencing analysis indicated that treatment did not consistently select for viral variants in NA. Furthermore, prophylactic administration of 3c10-3 did not inhibit the development of protective immunity to subsequent homologous virus re-challenge. Taken together, 3c10-3 highlights the potential use of anti-NA mAb to mitigate influenza virus infection.

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Comparative Efficacy of Monoclonal Antibodies That Bind to Different Epitopes of the 2009 Pandemic H1N1 Influenza Virus Neuraminidase

Cited by 50 publications

References 39 publications

Substrate Binding by the Second Sialic Acid-Binding Site of Influenza A Virus N1 Neuraminidase Contributes to Enzymatic Activity

Substrate Binding by the Second Sialic Acid-Binding Site of Influenza A Virus N1 Neuraminidase Contributes to Enzymatic Activity

Antibody neutralization of an influenza virus that uses neuraminidase for receptor binding

An influenza A virus (H7N9) anti-neuraminidase monoclonal antibody protects mice from morbidity without interfering with the development of protective immunity to subsequent homologous challenge

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