4.3 Article

Poor protective potential of influenza nucleoprotein antibodies despite wide prevalence

Journal

IMMUNOLOGY AND CELL BIOLOGY
Volume 100, Issue 1, Pages 49-60

Publisher

WILEY
DOI: 10.1111/imcb.12508

Keywords

antibody; humoral immunity; influenza virus; nucleoprotein

Funding

  1. Australian National Health and Medical Research Council [1052979]

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Humans are exposed to influenza virus and develop high levels of anti-NP antibodies, indicating NP as a major target of humoral immunity. Anti-NP human mAbs show potential for engaging in downstream Fc effector functions, but are not protective in vivo when passively transferred into a murine influenza challenge model. Further studies are needed to explore the synergistic effect of anti-NP mAbs with other influenza-specific mAbs.
Humans are exposed to influenza virus through periodic infections. Due to these repeated exposures, human populations commonly have elevated antibody titers targeting the conserved internal influenza virus nucleoprotein (NP). Despite the presence of anti-NP antibodies, humans are acutely susceptible to drifted influenza viruses with antigenically different surface proteins and the protective potential of human NP antibodies is unclear. In this study, high levels of anti-NP antibody and NP-specific B cells were detected in both adult humans and influenza-infected mice, confirming that NP is a major target of humoral immunity. Through sorting single B cells from influenza-exposed human adults, we generated a panel of 11 anti-NP monoclonal antibodies (mAbs). The majority of anti-NP human mAbs generated were capable of engaging cellular Fc receptors and bound NP on the surface of influenza-infected cell lines in vitro, suggesting that anti-NP mAbs have the potential to mediate downstream Fc effector functions such as antibody-dependent cellular cytotoxicity and antibody-dependent phagocytosis. However, human anti-NP mAbs were not protective in vivo when passively transferred into a murine influenza challenge model. Future in vivo studies examining the synergistic effect of anti-NP mAbs infused with other influenza-specific mAbs are warranted.

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