Abstract

We seek to understand the molecular basis of cell division, cytokinesis, in animal cells. The central spindle, a set of antiparallel bundled microtubules in the anaphase spindle, regulates formation of the actomyosin- based contractile ring and is essential for completion of cytokinesis. We propose that the organization and function of the central spindle is a consequence of the structural organization and biochemical properties of the centralspindlin complex. Centralspindlin is an evolutionary conserved, multimeric complex containing a kinesin-like protein (ZEN-4/MKLP1) and a Rho family GAP (CYK-4/MgcRacGAP) that is highly concentrated on the central spindle and midbody during anaphase and telophase, respectively. We propose to combine in vitro biochemistry and in vivo rescue assays in C. elegans embryos and in mammalian cells to address 3 specific aims: (1) To dissect the molecular organization of the centralspindlin complex and to characterize the atypical kinesin protein, ZEN-4. By characterizing the critical protein domains in the centralspindlin complex in relative isolation, we will develop the biochemical framework necessary to understand the function of these molecules in more complex reactions as well as in vivo. (2) To decipher the molecular mechanism of central spindle assembly. Central spindle assembly will be reconstituted in vitro from purified components in order to define the principles by which this set of dynamic components assemble into a highly ordered and stable structure. (3) To determine how the central spindle mediates completion of cytokinesis. Centralspindlin contains 2 distinct protein domains that are proposed to control late steps in cytokinesis. Therefore, the molecular function of these domains will be established. This research will provide molecular insights into a cellular structure that is critical for cell multiplication. Therefore, our research could contribute to the development of novel anti-mitotic agents for the treatment of cancer. Furthermore, molecular dissection of ZEN-4 will enhance our understanding of the mechanism of action of microtubule motors. ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
1R01GM074743-01A1
Application #
7093335
Study Section
Nuclear Dynamics and Transport (NDT)
Program Officer
Rodewald, Richard D
Project Start
2006-07-01
Project End
2010-06-30
Budget Start
2006-07-01
Budget End
2007-06-30
Support Year
1
Fiscal Year
2006
Total Cost
$284,566
Indirect Cost

  Institution

Name
University of Chicago
Department
Genetics
Type
Schools of Medicine
DUNS #
005421136
City
Chicago
State
IL
Country
United States
Zip Code
60637

  Publications

White, Erin A; Raghuraman, Hariharasundaram; Perozo, Eduardo et al. (2013) Binding of the CYK-4 subunit of the centralspindlin complex induces a large scale conformational change in the kinesin subunit. J Biol Chem 288:19785-95
White, Erin A; Glotzer, Michael (2012) Centralspindlin: at the heart of cytokinesis. Cytoskeleton (Hoboken) 69:882-92
Loria, Andy; Longhini, Katrina M; Glotzer, Michael (2012) The RhoGAP domain of CYK-4 has an essential role in RhoA activation. Curr Biol 22:213-9
Wolfe, Benjamin A; Takaki, Tohru; Petronczki, Mark et al. (2009) Polo-like kinase 1 directs assembly of the HsCyk-4 RhoGAP/Ect2 RhoGEF complex to initiate cleavage furrow formation. PLoS Biol 7:e1000110
Glotzer, Michael (2009) The 3Ms of central spindle assembly: microtubules, motors and MAPs. Nat Rev Mol Cell Biol 10:9-20
Glotzer, Michael (2009) Cytokinesis: GAP gap. Curr Biol 19:R162-5
Hutterer, Andrea; Glotzer, Michael; Mishima, Masanori (2009) Clustering of centralspindlin is essential for its accumulation to the central spindle and the midbody. Curr Biol 19:2043-9
Piekny, Alisa J; Glotzer, Michael (2008) Anillin is a scaffold protein that links RhoA, actin, and myosin during cytokinesis. Curr Biol 18:30-6
Kieserman, Esther K; Glotzer, Michael; Wallingford, John B (2008) Developmental regulation of central spindle assembly and cytokinesis during vertebrate embryogenesis. Curr Biol 18:116-23
Werner, Michael; Munro, Ed; Glotzer, Michael (2007) Astral signals spatially bias cortical myosin recruitment to break symmetry and promote cytokinesis. Curr Biol 17:1286-97

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