4.2 Article

Do nuclear envelope and intranuclear proteins reorganize during mitosis to form an elastic, hydrogel-like spindle matrix?

Journal

CHROMOSOME RESEARCH
Volume 19, Issue 3, Pages 345-365

Publisher

SPRINGER
DOI: 10.1007/s10577-011-9187-6

Keywords

spindle matrix; mitosis; nuclear reorganization; nuclear envelope; nucleoporins; microtubules

Funding

  1. NSF [MCB0817107]
  2. Div Of Molecular and Cellular Bioscience
  3. Direct For Biological Sciences [817107] Funding Source: National Science Foundation

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The idea of a spindle matrix has long been proposed in order to account for poorly understood features of mitosis. However, its molecular nature and structural composition have remained elusive. Here, we propose that the spindle matrix may be constituted by mainly nuclear-derived proteins that reorganize during the cell cycle to form an elastic gel-like matrix. We discuss this hypothesis in the context of recent observations from phylogenetically diverse organisms that nuclear envelope and intranuclear proteins form a highly dynamic and malleable structure that contributes to mitotic spindle function. We suggest that the viscoelastic properties of such a matrix may constrain spindle length while at the same time facilitating microtubule growth and dynamics as well as chromosome movement. A corollary to this hypothesis is that a key determinant of spindle size may be the amount of nuclear proteins available to form the spindle matrix. Such a matrix could also serve as a spatial regulator of spindle assembly checkpoint proteins during open and semi-open mitosis.

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