fumble Encodes a Pantothenate Kinase Homolog Required for Proper Mitosis and Meiosis in Drosophila melanogaster

fumble Encodes a Pantothenate Kinase Homolog Required for Proper Mitosis and Meiosis in Drosophila melanogaster

Katayoun Afshar^a, Pierre Gönczy^c, Stephen DiNardo^b, and Steven A. Wasserman^a
^a Center for Molecular Genetics, Division of Biology, University of California, San Diego, California 92093,
^b Department of Cell & Developmental Biology, University of Pennsylvania, Philadelphia, Pennsylvania 19104
^c The Rockefeller University, New York, New York 10021

Corresponding author: Katayoun Afshar, Center for Molecular Genetics, Division of Biology, University of California, 9500 Gilman Dr., San Diego, CA 92093-0634., kafshar{at}biomail.ucsd.edu (E-mail)

Communicating editor: R. S. HAWLEY

A number of fundamental processes comprise the cell divisioncycle, including spindle formation, chromosome segregation,and cytokinesis. Our current understanding of these processeshas benefited from the isolation and analysis of mutants, withthe meiotic divisions in the male germline of Drosophila beingparticularly well suited to the identification of the requiredgenes. We show here that the fumble (fbl) gene is required forcell division in Drosophila. We find that dividing cells infbl-deficient testes exhibit abnormalities in bipolar spindleorganization, chromosome segregation, and contractile ring formation.Cytological analysis of larval neuroblasts from null mutantsreveals a reduced mitotic index and the presence of polyploidcells. Molecular analysis demonstrates that fbl encodes threeprotein isoforms, all of which contain a domain with high similarityto the pantothenate kinases of A. nidulans and mouse. The largestFumble isoform is dispersed in the cytoplasm during interphase,concentrates around the spindle at metaphase, and localizesto the spindle midbody at telophase. During early embryonicdevelopment, the protein localizes to areas of membrane depositionand/or rearrangement, such as the metaphase and cellularizationfurrows. Given the role of pantothenate kinase in productionof Coenzyme A and in phospholipid biosynthesis, this patternof localization is suggestive of a role for fbl in membranesynthesis. We propose that abnormalities in synthesis and redistributionof membranous structures during the cell division cycle underliethe cell division defects in fbl mutant cells.

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