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Article
Mitotic Chromosome Condensation Mediated by the Retinoblastoma Protein Is Tumor-suppressive
Genes & Development
  • Courtney H. Coschi, The University of Western Ontario
  • Alison L. Martens, The University of Western Ontario
  • Kieran Ritchie, The University of Western Ontario
  • Sarah M. Francis, The University of Western Ontario
  • Subrata Chakrabarti, The University of Western Ontario
  • Nathalie G. Berube, The University of Western Ontario
  • Frederick A. Dick, The University of Western Ontario
Document Type
Article
Publication Date
7-1-2010
URL with Digital Object Identifier
http://dx.doi.org/10.1101/gad.1917610
Disciplines
Abstract

Condensation and segregation of mitotic chromosomes is a critical process for cellular propagation, and, in mammals, mitotic errors can contribute to the pathogenesis of cancer. In this report, we demonstrate that the retinoblastoma protein (pRB), a well-known regulator of progression through the G1 phase of the cell cycle, plays a critical role in mitotic chromosome condensation that is independent of G1-to-S-phase regulation. Using gene targeted mutant mice, we studied this aspect of pRB function in isolation, and demonstrate that it is an essential part of pRB-mediated tumor suppression. Cancer-prone Trp53(-/-) mice succumb to more aggressive forms of cancer when pRB's ability to condense chromosomes is compromised. Furthermore, we demonstrate that defective mitotic chromosome structure caused by mutant pRB accelerates loss of heterozygosity, leading to earlier tumor formation in Trp53(+/-) mice. These data reveal a new mechanism of tumor suppression, facilitated by pRB, in which genome stability is maintained by proper condensation of mitotic chromosomes.

Citation Information
Courtney H. Coschi, Alison L. Martens, Kieran Ritchie, Sarah M. Francis, et al.. "Mitotic Chromosome Condensation Mediated by the Retinoblastoma Protein Is Tumor-suppressive" Genes & Development Vol. 24 Iss. 13 (2010) p. 1351 - 1363
Available at: http://works.bepress.com/nathalie-berube/14/