Feo, the Drosophila Homolog of PRC1, Is Required for Central-Spindle Formation and Cytokinesis

We performed a functional analysis of fascetto (feo), a Drosophila gene that encodes a protein homologous to the Ase1p/PRC1/MAP65 conserved family of microtubule-associated proteins (MAPs) [1–5]. These MAPs are enriched at the spindle midzone in yeast and mammals and at the fragmoplast in plants, an...

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Bibliographic Details
Published in:Current biology 2004-09, Vol.14 (17), p.1569-1575
Main Authors: Vernı̀, Fiammetta, Somma, Maria Patrizia, Gunsalus, Kristin C., Bonaccorsi, Silvia, Belloni, Giorgio, Goldberg, Michael L., Gatti, Maurizio
Format: Article
Language:English
Subjects:
Animals
Base Sequence
Blotting, Western
Cell Cycle Proteins - genetics
Cell Cycle Proteins - physiology
Chromosome Mapping
Cytokinesis - genetics
Cytokinesis - physiology
DNA Primers
Drosophila
Drosophila - genetics
Drosophila - physiology
Drosophila Proteins - genetics
Drosophila Proteins - physiology
Female
Gene Components
Gene Expression
Immunohistochemistry
Male
Microtubule-Associated Proteins - genetics
Microtubule-Associated Proteins - physiology
Molecular Sequence Data
Mutation - genetics
Reverse Transcriptase Polymerase Chain Reaction
RNA Interference
Sequence Analysis, DNA
Sequence Homology
Sex Factors
Spermatocytes - metabolism
Spindle Apparatus - genetics
Spindle Apparatus - physiology
Transgenes - genetics
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Summary:We performed a functional analysis of fascetto (feo), a Drosophila gene that encodes a protein homologous to the Ase1p/PRC1/MAP65 conserved family of microtubule-associated proteins (MAPs) [1–5]. These MAPs are enriched at the spindle midzone in yeast and mammals and at the fragmoplast in plants, and are essential for the organization and function of these microtubule arrays [1–5]. Here we show that the Feo protein is specifically enriched at the central-spindle midzone and that its depletion either by mutation or by RNAi results in aberrant central spindles. In Feo-depleted cells, late anaphases showed normal overlap of the antiparallel MTs at the cell equator, but telophases displayed thin MT bundles of uniform width instead of robust hourglass-shaped central spindles. These thin central spindles exhibited diffuse localizations of both the Pav and Asp proteins, suggesting that these spindles comprise improperly oriented MTs. Feo-depleted cells also displayed defects in the contractile apparatus that correlated with those in the central spindle; late anaphase cells formed regular contractile structures, but these structures did not constrict during telophase, leading to failures in cytokinesis. The phenotype of Feo-depleted telophases suggests that Feo interacts with the plus ends of central spindle MTs so as to maintain their precise interdigitation during anaphase-telophase MT elongation and antiparallel sliding.
ISSN:0960-9822
1879-0445
DOI:10.1016/j.cub.2004.08.054