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    Date Issued2007 (1)2005 (1)Author
    Hergert, Polla J. (2)
    Delaval, Benedicte (1)Doxsey, Stephen J. (1)English, Christopher N. (1)Jurczyk, Agata (1)View MoreUMass Chan AffiliationDepartment of Cell Biology (1)Graduate School of Biomedical Sciences (1)Program in Molecular Medicine (1)Document TypeJournal Article (2)KeywordCell Biology (1)Cell Cycle (1)Cell Line; Cells, Cultured; Centrosome; Cyclin A; Cyclin-Dependent Kinase 2; Cyclin-Dependent Kinase Inhibitor p21; G1 Phase; Hela Cells; Humans; S Phase; Tumor Suppressor Protein p53; p38 Mitogen-Activated Protein Kinases (1)Centrioles (1)Genes, Reporter (1)View MoreJournalNature cell biology (1)The Journal of cell biology (1)

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    Loss of centrosome integrity induces p38-p53-p21-dependent G1-S arrest

    Mikule, Keith; Delaval, Benedicte; Kaldis, Philipp; Jurczyk, Agata; Hergert, Polla J.; Doxsey, Stephen J. (2007-03-03)
    Centrosomes organize the microtubule cytoskeleton for both interphase and mitotic functions. They are implicated in cell-cycle progression but the mechanism is unknown. Here, we show that depletion of 14 out of 15 centrosome proteins arrests human diploid cells in G1 with reduced Cdk2-cyclin A activity and that expression of a centrosome-disrupting dominant-negative construct gives similar results. Cell-cycle arrest is always accompanied by defects in centrosome structure and function (for example, duplication and primary cilia assembly). The arrest occurs from within G1, excluding contributions from mitosis and cytokinesis. The arrest requires p38, p53 and p21, and is preceded by p38-dependent activation and centrosomal recruitment of p53. p53-deficient cells fail to arrest, leading to centrosome and spindle dysfunction and aneuploidy. We propose that loss of centrosome integrity activates a checkpoint that inhibits G1-S progression. This model satisfies the definition of a checkpoint in having three elements: a perturbation that is sensed, a transducer (p53) and a receiver (p21).
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    The de novo centriole assembly pathway in HeLa cells: cell cycle progression and centriole assembly/maturation

    La Terra, Sabrina; English, Christopher N.; Hergert, Polla J.; McEwen, Bruce F.; Sluder, Greenfield; Khodjakov, Alexey (2005-03-02)
    It has been reported that nontransformed mammalian cells become arrested during G1 in the absence of centrioles (Hinchcliffe, E., F. Miller, M. Cham, A. Khodjakov, and G. Sluder. 2001. Science. 291:1547-1550). Here, we show that removal of resident centrioles (by laser ablation or needle microsurgery) does not impede cell cycle progression in HeLa cells. HeLa cells born without centrosomes, later, assemble a variable number of centrioles de novo. Centriole assembly begins with the formation of small centrin aggregates that appear during the S phase. These, initially amorphous "precentrioles" become morphologically recognizable centrioles before mitosis. De novo-assembled centrioles mature (i.e., gain abilities to organize microtubules and replicate) in the next cell cycle. This maturation is not simply a time-dependent phenomenon, because de novo-formed centrioles do not mature if they are assembled in S phase-arrested cells. By selectively ablating only one centriole at a time, we find that the presence of a single centriole inhibits the assembly of additional centrioles, indicating that centrioles have an activity that suppresses the de novo pathway.
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