| Literature DB >> 29746833 |
Kannan Tharakaraman1, Satoru Watanabe2, Kuan Rong Chan2, Jia Huan3, Vidya Subramanian1, Yok Hian Chionh4, Aditya Raguram5, Devin Quinlan1, Megan McBee4, Eugenia Z Ong2, Esther S Gan2, Hwee Cheng Tan2, Anu Tyagi3, Shashi Bhushan3, Julien Lescar3, Subhash G Vasudevan2, Eng Eong Ooi6, Ram Sasisekharan7.
Abstract
Following the recent emergence of Zika virus (ZIKV), many murine and human neutralizing anti-ZIKV antibodies have been reported. Given the risk of virus escape mutants, engineering antibodies that target mutationally constrained epitopes with therapeutically relevant potencies can be valuable for combating future outbreaks. Here, we applied computational methods to engineer an antibody, ZAb_FLEP, that targets a highly networked and therefore mutationally constrained surface formed by the envelope protein dimer. ZAb_FLEP neutralized a breadth of ZIKV strains and protected mice in distinct in vivo models, including resolving vertical transmission and fetal mortality in infected pregnant mice. Serial passaging of ZIKV in the presence of ZAb_FLEP failed to generate viral escape mutants, suggesting that its epitope is indeed mutationally constrained. A single-particle cryo-EM reconstruction of the Fab-ZIKV complex validated the structural model and revealed insights into ZAb_FLEP's neutralization mechanism. ZAb_FLEP has potential as a therapeutic in future outbreaks.Entities:
Keywords: ZIKV; Zika virus; antibody; cryo-EM; efficacy; flavivirus; neutralization; quaternary epitope; structure; therapeutic
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Year: 2018 PMID: 29746833 PMCID: PMC6018055 DOI: 10.1016/j.chom.2018.04.004
Source DB: PubMed Journal: Cell Host Microbe ISSN: 1931-3128 Impact factor: 21.023