5M5B

Crystal structure of Zika virus NS5 methyltransferase

Summary for 5M5B

• Entry DOI: 10.2210/pdb5m5b/pdb
• Descriptor: NS5 methyltransferase, S-ADENOSYLMETHIONINE, SULFATE ION, ... (6 entities in total)
• Functional Keywords: zika virus ns5 methyltransferase, transferase
• Biological source: Zika virus (ZIKV)
• Cellular location: Virion membrane ; Multi-pass membrane protein : H9A910
• Total number of polymer chains: 2
• Total formula weight: 61621.72

Authors

Barral, K.,Ortiz Lombardia, M.,Coutard, B.,Decroly, E.,Lichiere, J. (deposition date: 2016-10-21, release date: 2016-12-28, Last modification date: 2024-01-17)

Primary citation

Coutard, B.,Barral, K.,Lichiere, J.,Selisko, B.,Martin, B.,Aouadi, W.,Lombardia, M.O.,Debart, F.,Vasseur, J.J.,Guillemot, J.C.,Canard, B.,Decroly, E.
Zika Virus Methyltransferase: Structure and Functions for Drug Design Perspectives.
J. Virol., 91:-, 2017

PubMed Abstract: The Zika virus (ZIKV) is the causal agent of neurological disorders like microcephaly in newborns or Guillain-Barre syndrome. Its NS5 protein embeds a methyltransferase (MTase) domain involved in the formation of the viral mRNA cap. We investigated the structural and functional properties of the ZIKV MTase. We show that the ZIKV MTase can methylate RNA cap structures at the N-7 position of the cap, and at the 2'-O position on the ribose of the first nucleotide, yielding a cap-1 structure. In addition, the ZIKV MTase methylates the ribose 2'-O position of internal adenosines of RNA substrates. The crystal structure of the ZIKV MTase determined at a 2.01-Å resolution reveals a crystallographic homodimer. One chain is bound to the methyl donor (-adenosyl-l-methionine [SAM]) and shows a high structural similarity to the dengue virus (DENV) MTase. The second chain lacks SAM and displays conformational changes in the αX α-helix contributing to the SAM and RNA binding. These conformational modifications reveal a possible molecular mechanism of the enzymatic turnover involving a conserved Ser/Arg motif. In the second chain, the SAM binding site accommodates a sulfate close to a glycerol that could serve as a basis for structure-based drug design. In addition, compounds known to inhibit the DENV MTase show similar inhibition potency on the ZIKV MTase. Altogether these results contribute to a better understanding of the ZIKV MTase, a central player in viral replication and host innate immune response, and lay the basis for the development of potential antiviral drugs. The Zika virus (ZIKV) is associated with microcephaly in newborns, and other neurological disorders such as Guillain-Barre syndrome. It is urgent to develop antiviral strategies inhibiting the viral replication. The ZIKV NS5 embeds a methyltransferase involved in the viral mRNA capping process, which is essential for viral replication and control of virus detection by innate immune mechanisms. We demonstrate that the ZIKV methyltransferase methylates the mRNA cap and adenosines located in RNA sequences. The structure of ZIKV methyltransferase shows high structural similarities to the dengue virus methyltransferase, but conformational specificities highlight the role of a conserved Ser/Arg motif, which participates in RNA and SAM recognition during the reaction turnover. In addition, the SAM binding site accommodates a sulfate and a glycerol, offering structural information to initiate structure-based drug design. Altogether, these results contribute to a better understanding of the methyltransferases, which are central players in the virus replication.

PubMed: 28031359
DOI: 10.1128/JVI.02202-16

Experimental method

X-RAY DIFFRACTION (2.01 Å)