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AFMB, CNRS-Université de la Méditerranée
1 E-mail: barbara.selisko{at}afmb.univ-mrs.fr
The Flavivirus RNA genome contains a conserved cap-1 structure, 7MeGpppA2'OMeG, at the 5' end. Two mRNA cap methyltransferase (MTase) activites involved in the formation of the cap, the (guanine-N7) and the (nucleoside-2'O)-MTases, reside in a single domain of non-structural protein NS5 (NS5MTase). We report on the biochemical characterization of the 2'OMTase activity of NS5MTase of dengue virus (NS5MTaseDV) using purified short capped RNA substrates (7MeGpppACn or GpppACn). NS5MTaseDV methylates both types of substrate exclusively at the 2'O-position. The efficiency of 2'O-methylation does not depend on the methylation of the N7-position. Using 7MeGpppACn and GpppACn substrates of increasing chain lengths, we found that both NS5MTaseDV 2'O-activity and substrate binding increased before reaching a plateau at n=5. Thus the cap and 6 nucleotides might define the interface providing efficient binding of enzyme and substrate. Km values for 7MeGpppAC5 and the co-substrate S-adenosyl-L-methionine (AdoMet) were determined (0.39 and 3.26 ;micro;M, respectively). As other reported AdoMet-dependent RNA and DNA MTases, the 2'OMTase activity of NS5MTaseDV shows a low turnover of 3.25 x 10-4 s-1. Finally, we set up an inhibition assay and tested GTP- and AdoMet analogs as putative inhibitors of NS5MTaseDV. We confirmed efficient inhibition by the reaction product S-adenosyl-homocysteine (AdoHcy) (IC50 0.34 µM) and sinefungin (IC50 0.63 µM) demonstrating that the assay is sufficiently sensitive to conduct inhibitor screening and characterization assays.
Received 30 July 2009;
accepted 22 September 2009.
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| INT J SYST EVOL MICROBIOL | MICROBIOLOGY | J GEN VIROL |
| J MED MICROBIOL | ALL SGM JOURNALS | |
