The Drosophila Protein Asp Is Involved in Microtubule Organization during Spindle Formation and Cytokinesis

Abnormal spindle (Asp) is a 220-kD microtubule-associated protein from Drosophila that has been suggested to be involved in microtubule nucleation from the centrosome. Here, we show that Asp is enriched at the poles of meiotic and mitotic spindles and localizes to the minus ends of central spindle m...

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Bibliographic Details
Published in:The Journal of cell biology 2001-05, Vol.153 (4), p.637-647
Main Authors: Wakefield, James G., Bonaccorsi, Silvia, Gatti, Maurizio
Format: Article
Language:English
Subjects:
Animals
asp gene
Asp protein
asterless gene
Cell division
Cell Division - physiology
Cells
Cellular biology
Centrosome - metabolism
Centrosomes
Cytokinesis
Drosophila
Drosophila melanogaster
Drosophila Proteins
Embryos
Female
Male
Meiosis - physiology
Metaphase
Microtubule-Associated Proteins - genetics
Microtubule-Associated Proteins - metabolism
Microtubules
Mitotic spindle apparatus
Mutation
Mutation - physiology
Neurons
Neurons - cytology
Neurons - physiology
Original
Proteins
Spermatids - pathology
Spindle Apparatus - metabolism
Telophase
Telophase - physiology
Tubulin - metabolism
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Summary:Abnormal spindle (Asp) is a 220-kD microtubule-associated protein from Drosophila that has been suggested to be involved in microtubule nucleation from the centrosome. Here, we show that Asp is enriched at the poles of meiotic and mitotic spindles and localizes to the minus ends of central spindle microtubules. Localization to these structures is independent of a functional centrosome. Moreover, colchicine treatment disrupts Asp localization to the centrosome, indicating that Asp is not an integral centrosomal protein. In both meiotic and mitotic divisions of asp mutants, microtubule nucleation occurs from the centrosome, and γ-tubulin localizes correctly. However, spindle pole focusing and organization are severely affected. By examining cells that carry mutations both in asp and in asterless, a gene required for centrosome function, we have determined the role of Asp in the absence of centrosomes. Phenotypic analysis of these double mutants shows that Asp is required for the aggregation of microtubules into focused spindle poles, reinforcing the conclusion that its function at the spindle poles is independent of any putative role in microtubule nucleation. Our data also suggest that Asp has a role in the formation of the central spindle. The inability of asp mutants to correctly organize the central spindle leads to disruption of the contractile ring machinery and failure in cytokinesis.
ISSN:0021-9525
1540-8140
DOI:10.1083/jcb.153.4.637