Tracing the Origin of the Compensasome: Evolutionary History of DEAH Helicase and MYST Acetyltransferase Gene Families

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Molecular Biology and Evolution 18:330-343 (2001)
© 2001 Society for Molecular Biology and Evolution

ARTICLE

Tracing the Origin of the Compensasome: Evolutionary History of DEAH Helicase and MYST Acetyltransferase Gene Families

Rafael Sanjuán and Ignacio Marín²^,

Instituto Cavanilles de Biodiversidad y Biología Evolutiva and Departamento de Genética, Universidad de Valencia, Spain

Dosage compensation in Drosophila is mediated by a complex ofproteins and RNAs called the "compensasome." Two of the genesthat encode proteins of the complex, maleless (mle) and males-absent-on-the-first(mof), respectively, belong to the DEAH helicase and MYST acetyltransferasegene families. We performed comprehensive phylogenetic and structuralanalyses to determine the evolutionary histories of these twogene families and thus to better understand the origin of thecompensasome. All of the members of the DEAH and MYST familiesof the completely sequenced Saccharomyces cerevisiae and Caenorhabditiselegans genomes, as well as those so far (June 2000) found inDrosophila melanogaster (for which the euchromatic part of thegenome has also been fully sequenced) and Homo sapiens, wereanalyzed. We describe a total of 39 DEAH helicases in thesefour species. Almost all of them can be grouped in just threemain branches. The first branch includes the yeast PRP2, PRP16,PRP22, and PRP43 splicing factors and their orthologs in animalspecies. Each PRP gene has a single ortholog in metazoans. Thesecond branch includes just four genes, found in yeast (Ecm16)and Drosophila (kurz) and their orthologs in humans and Caenorhabditis.The third branch includes (1) a single yeast gene (YLR419w);(2) six Drosophila genes, including maleless and spindle-E/homeless;(3) four human genes, among them the ortholog of maleless, whichencodes RNA helicase A; and (4) three C. elegans genes, includingorthologs of maleless and spindle-E. Thus, this branch has largelyexpanded in metazoans. We also show that, for the whole DEAHfamily, only MLE and its metazoan orthologs have acquired newprotein domains since the fungi/animals split. We found a totalof 17 MYST family proteins in the four analyzed species. Wedetermined putative orthologs of mof in both C. elegans andH. sapiens, and we show that the most likely ortholog in yeastis the Sas2 gene. Moreover, a paralog of mof exists in Drosophila.All of these results, together with those found for a thirdmember of the compensasome, msl-3, suggest that this complexemerged after the fungi/animals split and that it may be presentin mammalian species. Both gene duplication and the acquisitionof new protein modules may have played important roles in theorigin of the compensasome.

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