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      Functional Characterization of Adaptive Mutations during the West African Ebola Virus Outbreak.

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          Abstract

          The Ebola virus (EBOV) outbreak in West Africa started in December 2013, claimed more than 11,000 lives, threatened to destabilize a whole region, and showed how easily health crises can turn into humanitarian disasters. EBOV genomic sequences of the West African outbreak revealed nonsynonymous mutations, which induced considerable public attention, but their role in virus spread and disease remains obscure. In this study, we investigated the functional significance of three nonsynonymous mutations that emerged early during the West African EBOV outbreak. Almost 90% of more than 1,000 EBOV genomes sequenced during the outbreak carried the signature of three mutations: a D759G substitution in the active center of the L polymerase, an A82V substitution in the receptor binding domain of surface glycoprotein GP, and an R111C substitution in the self-assembly domain of RNA-encapsidating nucleoprotein NP. Using a newly developed virus-like particle system and reverse genetics, we found that the mutations have an impact on the functions of the respective viral proteins and on the growth of recombinant EBOVs. The mutation in L increased viral transcription and replication, whereas the mutation in NP decreased viral transcription and replication. The mutation in the receptor binding domain of the glycoprotein GP improved the efficiency of GP-mediated viral entry into target cells. Recombinant EBOVs with combinations of the three mutations showed a growth advantage over the prototype isolate Makona C7 lacking the mutations. This study showed that virus variants with improved fitness emerged early during the West African EBOV outbreak.

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          Author and article information

          Journal
          J. Virol.
          Journal of virology
          American Society for Microbiology
          1098-5514
          0022-538X
          Jan 15 2017
          : 91
          : 2
          Affiliations
          [1 ] Institute of Virology, Philipps University Marburg, Marburg, Germany.
          [2 ] German Center for Infection Research, Site Gießen-Marburg-Langen, Marburg, Germany.
          [3 ] Institute of Virology, Philipps University Marburg, Marburg, Germany becker@staff.uni-marburg.de.
          Article
          JVI.01913-16
          10.1128/JVI.01913-16
          5215343
          27847361
          83635e76-1d0e-4f77-9247-c1e7a901fdd6
          History

          adaptive mutations,Ebola virus,West Africa,glycoprotein,zoonotic infections

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