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Pmt1, a Dnmt2 homolog in Schizosaccharomyces pombe,mediates tRNA methylation in response to nutrient signaling
Authors:Maria Becker  Sara Müller  Wolfgang Nellen  Tomasz P. Jurkowski  Albert Jeltsch  Ann E. Ehrenhofer-Murray
Affiliation:1.Zentrum für Medizinische Biotechnologie, Universität Duisburg-Essen, 45117 Essen, 2.Abteilung Genetik, Universität Kassel, 34132 Kassel and 3.Institute of Biochemistry, Universität Stuttgart, 70569 Stuttgart, Germany
Abstract:The fission yeast Schizosaccharomyces pombe carries a cytosine 5-methyltransferase homolog of the Dnmt2 family (termed pombe methyltransferase 1, Pmt1), but contains no detectable DNA methylation. Here, we found that Pmt1, like other Dnmt2 homologs, has in vitro methylation activity on cytosine 38 of tRNAAsp and, to a lesser extent, of tRNAGlu, despite the fact that it contains a non-consensus residue in catalytic motif IV as compared with its homologs. In vivo tRNA methylation also required Pmt1. Unexpectedly, however, its in vivo activity showed a strong dependence on the nutritional status of the cell because Pmt1-dependent tRNA methylation was induced in cells grown in the presence of peptone or with glutamate as a nitrogen source. Furthermore, this induction required the serine/threonine kinase Sck2, but not the kinases Sck1, Pka1 or Tor1 and was independent of glucose signaling. Taken together, this work reveals a novel connection between nutrient signaling and tRNA methylation that thus may link tRNA methylation to processes downstream of nutrient signaling like ribosome biogenesis and translation initiation.
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