Literature DB >> 11343773

Correlation between centrosome abnormalities and chromosomal instability in human pancreatic cancer cells.

N Sato1, K Mizumoto, M Nakamura, N Maehara, Y A Minamishima, S Nishio, E Nagai, M Tanaka.   

Abstract

Chromosomal instability, characterized by abnormal numbers or structures of chromosomes, is a common feature of human cancers, but the mechanisms behind these changes are still unclear. Since centrosomes play a pivotal role in balanced chromosomal segregation during mitosis, we attempted to investigate the association between centrosome abnormalities and chromosomal instability in a large number of human pancreatic cancer cell lines. Immunofluorescence microscopy revealed centrosomes that were highly atypical with respect to their size, shape, and number in most cell lines. These abnormal centrosomes contributed to the assembly of multipolar spindles, resulting in defective mitosis and chromosome mis-segregation. Interestingly, a high frequency of centrosome defects inversely correlated with the growth rate of cells in culture. Fluorescence in situ hybridization revealed a dramatic variation of chromosome numbers in cell lines with the defective centrosome phenotype. Furthermore, a significant positive correlation existed between the level of centrosome defects and the level of chromosomal imbalances. These results indicate that centrosome abnormalities can lead to spindle disorganization and chromosome segregation errors, which may drive the accumulation of chromosomal alterations. Thus, defects in centrosome function may be an underlying cause of genetic instability in human pancreatic cancers.

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Year:  2001        PMID: 11343773     DOI: 10.1016/s0165-4608(00)00384-8

Source DB:  PubMed          Journal:  Cancer Genet Cytogenet        ISSN: 0165-4608


  29 in total

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4.  Amplified centrosomes may underlie aggressive disease course in pancreatic ductal adenocarcinoma.

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Authors:  Fergus J Couch; Xianshu Wang; William R Bamlet; Mariza de Andrade; Gloria M Petersen; Robert R McWilliams
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7.  Multipolar spindle pole coalescence is a major source of kinetochore mis-attachment and chromosome mis-segregation in cancer cells.

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8.  USP33 regulates centrosome biogenesis via deubiquitination of the centriolar protein CP110.

Authors:  Ji Li; Vincenzo D'Angiolella; E Scott Seeley; Sehyun Kim; Tetsuo Kobayashi; Wenxiang Fu; Eric I Campos; Michele Pagano; Brian David Dynlacht
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9.  Nucleation capacity and presence of centrioles define a distinct category of centrosome abnormalities that induces multipolar mitoses in cancer cells.

Authors:  Michael J Difilippantonio; B Michael Ghadimi; Tamara Howard; Jordi Camps; Quang Tri Nguyen; Douglas K Ferris; Dan L Sackett; Thomas Ried
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10.  A mechanism linking extra centrosomes to chromosomal instability.

Authors:  Neil J Ganem; Susana A Godinho; David Pellman
Journal:  Nature       Date:  2009-06-07       Impact factor: 49.962

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