DOT1A-dependent H3K76 methylation is required for replication regulation in Trypanosoma brucei |
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| Authors: | Alwine Gassen Doris Brechtefeld Niklas Schandry J. Manuel Arteaga-Salas Lars Israel Axel Imhof Christian J. Janzen |
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| Affiliation: | 1Department of Biology I, University of Munich (LMU), Genetics, Großhaderner Str. 2-4, 82152 Martinsried and 2Department of Molecular Biology, University of Munich (LMU), Adolf Butenandt Institute, Schillerstr. 44, 80336 Munich, Germany |
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| Abstract: | Cell-cycle progression requires careful regulation to ensure accurate propagation of genetic material to the daughter cells. Although many cell-cycle regulators are evolutionarily conserved in the protozoan parasite Trypanosoma brucei, novel regulatory mechanisms seem to have evolved. Here, we analyse the function of the histone methyltransferase DOT1A during cell-cycle progression. Over-expression of DOT1A generates a population of cells with aneuploid nuclei as well as enucleated cells. Detailed analysis shows that DOT1A over-expression causes continuous replication of the nuclear DNA. In contrast, depletion of DOT1A by RNAi abolishes replication but does not prevent karyokinesis. As histone H3K76 methylation has never been associated with replication control in eukaryotes before, we have discovered a novel function of DOT1 enzymes, which might not be unique to trypanosomes. |
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