Structural Basis of Zika Virus Specific Neutralization in Subsequent Flavivirus Infections

Author:

Sevvana MadhumatiORCID,Rogers Thomas F.,Miller Andrew S.,Long Feng,Klose ThomasORCID,Beutler NathanORCID,Lai Yen-Chung,Parren MaraORCID,Walker Laura M.,Buda Geeta,Burton Dennis R.,Rossmann Michael G.,Kuhn Richard J.

Abstract

Zika virus (ZIKV), a mosquito-borne human flavivirus that causes microcephaly and other neurological disorders, has been a recent focus for the development of flavivirus vaccines and therapeutics. We report here a 4.0 Å resolution structure of the mature ZIKV in complex with ADI-30056, a ZIKV-specific human monoclonal antibody (hMAb) isolated from a ZIKV infected donor with a prior dengue virus infection. The structure shows that the hMAb interactions span across the E protein dimers on the virus surface, inhibiting conformational changes required for the formation of infectious fusogenic trimers similar to the hMAb, ZIKV-117. Structure-based functional analysis, and structure and sequence comparisons, identified ZIKV residues essential for neutralization and crucial for the evolution of highly potent E protein crosslinking Abs in ZIKV. Thus, this epitope, ZIKV’s “Achilles heel”, defined by the contacts between ZIKV and ADI-30056, could be a suitable target for the design of therapeutic antibodies.

Publisher

MDPI AG

Subject

Virology,Infectious Diseases

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