Structure and Function of Flavivirus NS5 Methyltransferase

Zhou, Y; Ray, D; Zhao, Y; Dong, H; Ren, S; Li, Z; Guo, Y; Bernard, K; Shi, P; Li, H

doi:10.1128/JVI.02704-06

Title: Structure and Function of Flavivirus NS5 Methyltransferase

Journal Article · Mon Jan 01 00:00:00 EST 2007 · Journal of Virology

DOI:https://doi.org/10.1128/JVI.02704-06· OSTI ID:930027

Zhou, Y; Ray, D; Zhao, Y; Dong, H; Ren, S; Li, Z; Guo, Y; Bernard, K; Shi, P; Li, H

The plus-strand RNA genome of flavivirus contains a 5' terminal cap 1 structure (m{sup 7}GpppAmG). The flaviviruses encode one methyltransferase, located at the N-terminal portion of the NS5 protein, to catalyze both guanine N-7 and ribose 2'-OH methylations during viral cap formation. Representative flavivirus methyltransferases from dengue, yellow fever, and West Nile virus (WNV) sequentially generate GpppA {yields} m{sup 7}GpppA {yields} m{sup 7}GpppAm. The 2'-O methylation can be uncoupled from the N-7 methylation, since m{sup 7}GpppA-RNA can be readily methylated to m{sup 7}GpppAm-RNA. Despite exhibiting two distinct methylation activities, the crystal structure of WNV methyltransferase at 2.8 {angstrom} resolution showed a single binding site for S-adenosyl-L-methionine (SAM), the methyl donor. Therefore, substrate GpppA-RNA should be repositioned to accept the N-7 and 2'-O methyl groups from SAM during the sequential reactions. Electrostatic analysis of the WNV methyltransferase structure showed that, adjacent to the SAM-binding pocket, is a highly positively charged surface that could serve as an RNA binding site during cap methylations. Biochemical and mutagenesis analyses show that the N-7 and 2'-O cap methylations require distinct buffer conditions and different side chains within the K{sub 61}-D{sub 146}-K{sub 182}-E{sub 218} motif, suggesting that the two reactions use different mechanisms. In the context of complete virus, defects in both methylations are lethal to WNV; however, viruses defective solely in 2'-O methylation are attenuated and can protect mice from later wild-type WNV challenge. The results demonstrate that the N-7 methylation activity is essential for the WNV life cycle and, thus, methyltransferase represents a novel target for flavivirus therapy.

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Research Organization:: Brookhaven National Lab. (BNL), Upton, NY (United States). National Synchrotron Light Source

Sponsoring Organization:: Doe - Office Of Science

DOE Contract Number:: DE-AC02-98CH10886

OSTI ID:: 930027

Report Number(s):: BNL-80641-2008-JA; JOVIAM; TRN: US200822%%1263

Journal Information:: Journal of Virology, Vol. 81; ISSN 0022-538X

Country of Publication:: United States

Language:: English

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36 MATERIALS SCIENCE
BUFFERS
CRYSTAL STRUCTURE
DEFECTS
ELECTROSTATICS
FEVER
FUNCTIONS
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LETHAL MUTATIONS
LIFE CYCLE
METHYLATION
MICE
MUTAGENESIS
RESOLUTION
RIBOSE
RNA
SUBSTRATES
SURFACES
THERAPY
VIRUSES
national synchrotron light source

Title: Structure and Function of Flavivirus NS5 Methyltransferase

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