Characterization of HCP-6, a C. elegans protein required to prevent chromosome twisting and merotelic attachment

Jeffrey H. Stear; Mark B. Roth

doi:10.1101/gad.989102

Characterization of HCP-6, a C. elegans protein required to prevent chromosome twisting and merotelic attachment

Jeffrey H. Stear1,2 and
Mark B. Roth1,3

¹Division of Basic Sciences, Fred Hutchinson Cancer Research Center, Seattle, Washington 98109, USA; ²Molecular and Cellular Biology Program, University of Washington, Seattle, Washington 98195, USA

Abstract

Previous studies of mitosis show that capture of single kinetochores by microtubules from both centrosomes (merotelic orientation) is a major cause of aneuploidy. We have characterized hcp-6, a temperature-sensitive chromosome segregation mutant in C. elegans that exhibits chromosomes attached to both poles via a single sister kinetochore. We demonstrate that the primary defect in this mutant is a failure to fully condense chromosomes during prophase. Although centromere formation and sister centromere resolution remain unaffected in hcp-6, the chromosomes lack the rigidity of wild-type chromosomes and twist around the long axis of the chromosome. As such, they are unable to establish a proper orientation at prometaphase, allowing individual kinetochores to be captured by microtubules from both poles. We therefore propose that chromosome rigidity plays an essential role in maintaining chromosome orientation to prevent merotelic capture.

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Footnotes

↵3 Corresponding author.
E-MAIL mroth{at}fred.fhcrc.org; FAX (206) 667-6877.
Article and publication are at http://www.genesdev.org/cgi/doi/10.1101/gad.989102.
- Received March 4, 2002.
- Accepted April 29, 2002.
Cold Spring Harbor Laboratory Press