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A Novel Mammalian, Mitotic Spindle-Associated Kinase Is Related to Yeast and Fly Chromosome Segregation Regulators

  1. Author:
    Gopalan, G.
    Chan, C. S. M.
    Donovan, P. J.
  2. Author Address

    Donovan PJ NCI FREDERICK CANC RES & DEV CTR ABL BASIC RES PROGRAM CELL BIOL DEV & DIFFERENTIAT GRP FREDERICK, MD 21702 USA NCI FREDERICK CANC RES & DEV CTR ABL BASIC RES PROGRAM CELL BIOL DEV & DIFFERENTIAT GRP FREDERICK, MD 21702 USA UNIV TEXAS DEPT MICROBIOL AUSTIN, TX 78712 USA
    1. Year: 1997
  1. Journal: Journal of Cell Biology
    1. 138
    2. 3
    3. Pages: 643-656
  2. Type of Article: Article
  1. Abstract:

    We describe a novel mammalian protein kinase related to two newly identified yeast and fly kinases-Ipl1 and aurora, respectively-mutations in which cause disruption of chromosome segregation. We have designated this kinase as Ipl1- and aurora-related kinase 1 (IAK1). IAK1 expression in mouse fibroblasts is tightly regulated temporally and spatially during the cell cycle. Transcripts first appear at G(1)/S boundary, are elevated at M-phase, and disappear rapidly after completion of mitosis. The protein levels and kinase activity of IAK1 are also cell cycle regulated with a peak at M-phase. IAK1 protein has a distinct subcellular and temporal pattern of localization. It is first identified on the centrosomes immediately after the duplicated centrosomes have separated. The protein remains on the centrosome and the centrosome-proximal part of the spindle throughout mitosis and is detected weakly on midbody microtubules at telophase and cytokinesis, In cells recovering from nocodazole treatment and in taxol-treated mitotic cells, IAK1 is associated with microtubule organizing centers. A wild-type and a mutant form of IAK1 cause mitotic spindle defects and lethality in ipl1 mutant yeast cells but not in wild-type cells, suggesting that IAK1 interferes with Ipl1p function in yeast. Taken together, these data strongly suggest that IAK1 may have an important role in centrosome and/or spindle function during chromosome segregation in mammalian cells. We suggest that IAK1 is a new member of an emerging subfamily of the serine/threonine kinase superfamily. The members of this subfamily may be important regulators of chromosome segregation. [References: 37]

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