Biomolecules (May 2018)

Structural Transition and Antibody Binding of EBOV GP and ZIKV E Proteins from Pre-Fusion to Fusion-Initiation State

  • Anna Lappala,
  • Wataru Nishima,
  • Jacob Miner,
  • Paul Fenimore,
  • Will Fischer,
  • Peter Hraber,
  • Ming Zhang,
  • Benjamin McMahon,
  • Chang-Shung Tung

DOI
https://doi.org/10.3390/biom8020025
Journal volume & issue
Vol. 8, no. 2
p. 25

Abstract

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Membrane fusion proteins are responsible for viral entry into host cells—a crucial first step in viral infection. These proteins undergo large conformational changes from pre-fusion to fusion-initiation structures, and, despite differences in viral genomes and disease etiology, many fusion proteins are arranged as trimers. Structural information for both pre-fusion and fusion-initiation states is critical for understanding virus neutralization by the host immune system. In the case of Ebola virus glycoprotein (EBOV GP) and Zika virus envelope protein (ZIKV E), pre-fusion state structures have been identified experimentally, but only partial structures of fusion-initiation states have been described. While the fusion-initiation structure is in an energetically unfavorable state that is difficult to solve experimentally, the existing structural information combined with computational approaches enabled the modeling of fusion-initiation state structures of both proteins. These structural models provide an improved understanding of four different neutralizing antibodies in the prevention of viral host entry.

Keywords