Molecular Cloning and Tissue-Specific Expression of the mutator2 Gene (mu2) in Drosophila melanogaster

Molecular Cloning and Tissue-Specific Expression of the mutator2 Gene (mu2) in Drosophila melanogaster

Armin Kasravi^a, Marika F. Walter^a, Stephanie Brand^c, James M. Mason^b, and Harald Biessmann^a
^a Developmental Biology Center, University of California, Irvine, California 92697,
^b Department of Anatomy and Physiology, University of Dundee, Dundee DD1 4HN, Scotland
^c Laboratory of Molecular Genetics, National Institute of Environmental Health Sciences, Research Triangle Park, North Carolina 27709

Corresponding author: Harald Biessmann, Developmental Biology Center, University of California, Irvine, CA 92697., hbiessma{at}uci.edu (E-mail)

Communicating editor: R. S. HAWLEY

We present here the molecular cloning and characterization ofthe mutator2 (mu2) gene of Drosophila melanogaster togetherwith further genetic analyses of its mutant phenotype. mu2 functionsin oogenesis during meiotic recombination, during repair ofradiation damage in mature oocytes, and in proliferating somaticcells, where mu2 mutations cause an increase in somatic recombination.Our data show that mu2 represents a novel component in the processingof double strand breaks (DSBs) in female meiosis. mu2 does notcode for a DNA repair enzyme because mu2 mutants are not hypersensitiveto DSB-inducing agents. We have mapped and cloned the mu2 geneand rescued the mu2 phenotype by germ-line transformation withgenomic DNA fragments containing the mu2 gene. Sequencing itscDNA demonstrates that mu2 encodes a novel 139-kD protein, whichis highly basic in the carboxy half and carries three nuclearlocalization signals and a helix-loop-helix domain. Consistentwith the sex-specific mutant phenotype, the gene is expressedin ovaries but not in testes. During oogenesis its RNA is rapidlytransported from the nurse cells into the oocyte where it accumulatesspecifically at the anterior margin. Expression is also prominentin diploid proliferating cells of larval somatic tissues. Ourgenetic and molecular data are consistent with the model thatmu2 encodes a structural component of the oocyte nucleus. TheMU2 protein may be involved in controlling chromatin structureand thus may influence the processing of DNA DSBs.

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