An active site mutation increases the polymerase activity of the guinea pig-lethal Marburg virus | Zendy

Alexander Koehler | Zendy; Larissa Kolesnikova | Zendy; Stephan Becker | Zendy

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An active site mutation increases the polymerase activity of the guinea pig-lethal Marburg virus

Author(s) -

Alexander Koehler,

Larissa Kolesnikova,

Stephan Becker

Publication year - 2016

Publication title -

journal of general virology

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 1.55

H-Index - 167

eISSN - 1465-2099

pISSN - 0022-1317

DOI - 10.1099/jgv.0.000564

Subject(s) - biology , virology , polymerase , marburg virus , virus , viral replication , mutant , rna polymerase , microbiology and biotechnology , guinea pig , transcription (linguistics) , mutation , rna , gene , genetics , ebola virus , linguistics , philosophy

Marburg virus (MARV) causes severe, often fatal, disease in humans and transient illness in rodents. Sequential passaging of MARV in guinea pigs resulted in selection of a lethal virus containing 4 aa changes. A D184N mutation in VP40 (VP40D184N), which leads to a species-specific gain of viral fitness, and three mutations in the active site of viral RNA-dependent RNA polymerase L, which were investigated in the present study for functional significance in human and guinea pig cells. The transcription/replication activity of L mutants was strongly enhanced by a substitution at position 741 (S741C), and inhibited by other substitutions (D758A and A759D) in both species. The polymerase activity of L carrying the S741C substitution was eightfold higher in guinea pig cells than in human cells upon co-expression with VP40D184N, suggesting that the additive effect of the two mutations provides MARV a replicative advantage in the new host.

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