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Nucl._Acids_Res.-2013-El_Omari-9396-410.pdf (21.22 MB)

Tracking in atomic detail the functional specializations in viral RecA helicases that occur during evolution

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posted on 2023-06-08, 20:34 authored by Kamel El Omari, Christoph Meier, Denis Kainov, Geoff Sutton, Jonathan M Grimes, Minna M Poranen, Dennis H Bamford, Roman Tuma, David I Stuart, Erika ManciniErika Mancini
Many complex viruses package their genomes into empty protein shells and bacteriophages of the Cystoviridae family provide some of the simplest models for this. The cystoviral hexameric NTPase, P4, uses chemical energy to translocate single-stranded RNA genomic precursors into the procapsid. We previously dissected the mechanism of RNA translocation for one such phage, 12, and have now investigated three further highly divergent, cystoviral P4 NTPases (from 6, 8 and 13). High-resolution crystal structures of the set of P4s allow a structure-based phylogenetic analysis, which reveals that these proteins form a distinct subfamily of the RecA-type ATPases. Although the proteins share a common catalytic core, they have different specificities and control mechanisms, which we map onto divergent N- and C-terminal domains. Thus, the RNA loading and tight coupling of NTPase activity with RNA translocation in 8 P4 is due to a remarkable C-terminal structure, which wraps right around the outside of the molecule to insert into the central hole where RNA binds to coupled L1 and L2 loops, whereas in 12 P4, a C-terminal residue, serine 282, forms a specific hydrogen bond to the N7 of purines ring to confer purine specificity for the 12 enzyme.

History

Publication status

  • Published

File Version

  • Published version

Journal

Nucleic Acids Research

ISSN

1362-4962

Publisher

Oxford University Press

Issue

20

Volume

41

Page range

9396-9410

Department affiliated with

  • Biochemistry Publications

Full text available

  • Yes

Peer reviewed?

  • Yes

Legacy Posted Date

2015-04-22

First Open Access (FOA) Date

2015-04-22

First Compliant Deposit (FCD) Date

2015-04-22

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