Literature DB >> 20551165

Loss of pRB causes centromere dysfunction and chromosomal instability.

Amity L Manning1, Michelle S Longworth, Nicholas J Dyson.   

Abstract

Chromosome instability (CIN) is a common feature of tumor cells. By monitoring chromosome segregation, we show that depletion of the retinoblastoma protein (pRB) causes rates of missegregation comparable with those seen in CIN tumor cells. The retinoblastoma tumor suppressor is frequently inactivated in human cancers and is best known for its regulation of the G1/S-phase transition. Recent studies have shown that pRB inactivation also slows mitotic progression and promotes aneuploidy, but reasons for these phenotypes are not well understood. Here we describe the underlying mitotic defects of pRB-deficient cells that cause chromosome missegregation. Analysis of mitotic cells reveals that pRB depletion compromises centromeric localization of CAP-D3/condensin II and chromosome cohesion, leading to an increase in intercentromeric distance and deformation of centromeric structure. These defects promote merotelic attachment, resulting in failure of chromosome congression and an increased propensity for lagging chromosomes following mitotic delay. While complete loss of centromere function or chromosome cohesion would have catastrophic consequences, these more moderate defects allow pRB-deficient cells to proliferate but undermine the fidelity of mitosis, leading to whole-chromosome gains and losses. These observations explain an important consequence of RB1 inactivation, and suggest that subtle defects in centromere function are a frequent source of merotely and CIN in cancer.

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Year:  2010        PMID: 20551165      PMCID: PMC2895196          DOI: 10.1101/gad.1917310

Source DB:  PubMed          Journal:  Genes Dev        ISSN: 0890-9369            Impact factor:   11.361


  61 in total

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Authors:  Helen Dimaras; Vikas Khetan; William Halliday; Marija Orlic; Nadia L Prigoda; Beata Piovesan; Paula Marrano; Timothy W Corson; Ralph C Eagle; Jeremy A Squire; Brenda L Gallie
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Journal:  Nat Genet       Date:  2003-08       Impact factor: 38.330

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Authors:  D Cimini; B Howell; P Maddox; A Khodjakov; F Degrassi; E D Salmon
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  116 in total

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6.  Targeting tumor suppressor networks for cancer therapeutics.

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Review 7.  Too much to handle - how gaining chromosomes destabilizes the genome.

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8.  Disruption of CDK-resistant chromatin association by pRB causes DNA damage, mitotic errors, and reduces Condensin II recruitment.

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9.  Loss of RBF1 changes glutamine catabolism.

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Journal:  Genes Dev       Date:  2013-01-15       Impact factor: 11.361

10.  Cyclin E2 induces genomic instability by mechanisms distinct from cyclin E1.

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