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Neuraminidase inhibition contributes to influenza A virus neutralization by anti-hemagglutinin stem antibodies.


ABSTRACT: Broadly neutralizing antibodies (Abs) that bind the influenza virus hemagglutinin (HA) stem may enable universal influenza vaccination. Here, we show that anti-stem Abs sterically inhibit viral neuraminidase (NA) activity against large substrates, with activity inversely proportional to the length of the fibrous NA stalk that supports the enzymatic domain. By modulating NA stalk length in recombinant IAVs, we show that anti-stem Abs inhibit virus release from infected cells by blocking NA, accounting for their in vitro neutralization activity. NA inhibition contributes to anti-stem Ab protection in influenza-infected mice, likely due at least in part to NA-mediated inhibition of Fc?R-dependent activation of innate immune cells by Ab bound to virions. Food and Drug Administration-approved NA inhibitors enhance anti-stem-based Fc-dependent immune cell activation, raising the possibility of therapeutic synergy between NA inhibitors and anti-stem mAb treatment in humans.

SUBMITTER: Kosik I 

PROVIDER: S-EPMC6363425 | biostudies-literature | 2019 Feb

REPOSITORIES: biostudies-literature

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Neuraminidase inhibition contributes to influenza A virus neutralization by anti-hemagglutinin stem antibodies.

Kosik Ivan I   Angeletti Davide D   Gibbs James S JS   Angel Matthew M   Takeda Kazuyo K   Kosikova Martina M   Nair Vinod V   Hickman Heather D HD   Xie Hang H   Brooke Christopher B CB   Yewdell Jonathan W JW  

The Journal of experimental medicine 20190125 2


Broadly neutralizing antibodies (Abs) that bind the influenza virus hemagglutinin (HA) stem may enable universal influenza vaccination. Here, we show that anti-stem Abs sterically inhibit viral neuraminidase (NA) activity against large substrates, with activity inversely proportional to the length of the fibrous NA stalk that supports the enzymatic domain. By modulating NA stalk length in recombinant IAVs, we show that anti-stem Abs inhibit virus release from infected cells by blocking NA, accou  ...[more]

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