Centrosomal abnormalities, multipolar mitoses, and chromosomal instability in head and neck tumours with dysfunctional telomeres

Gisselsson, David; Jonson, Tord; Yu, Chiang; Martins, Conceição; Mandahl, Nils; Wiegant, J.; Jin, Yuesheng; Mertens, Fredrik; Jin, Charlotte

doi:10.1038/sj.bjc.6600438

Cited by 85 publications

(81 citation statements)

References 31 publications

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“…Furthermore, all MMs that were analyzed by immunofluorescence in the present study showed two or more centrosomes. The frequencies of AB and MM are positively correlated in many types of neoplasia (20,34,35). In the present study, MM was never present in the cultured WT cells or tissue sections without AB being present as well.…”

Section: Discussioncontrasting

confidence: 47%

Defective Chromosome Segregation and Telomere Dysfunction in Aggressive Wilms' Tumors

Stewénius¹,

Jin²,

Øra

et al. 2007

Clinical Cancer Research

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Purpose: In many childhood neoplasms, prognostic subgroups have been defined based on specific chromosome changes. In Wilms' tumor (WT), such subclassification has been hampered by the diverse and relatively unspecific pattern of chromosomal imbalances present in these tumors. Unspecific patterns of cytogenetic imbalances in tumors are often caused by mitotic segregation errors due to short dysfunctional telomeres. As an alternative to cytogenetic classification, we therefore have evaluated whether the rate of telomere-dependent chromosomal instability could influence the clinical course in WT patients. Experimental Design: Telomere function and mitotic segregation errors were assessed in 12 cultured tumors and in tumor tissue sections from 41WT patients. Results: Abnormal telomere shortening was found in cultured cells and in tissue sections from highly aggressive tumors. In vitro, dysfunctional telomeres were associated to specific cell division abnormalities, including anaphase bridges and multipolar mitoses. Assessment of mitotic figures in tissue sections revealed that anaphase bridges and multipolar mitoses were predominantly, but not exclusively, present in high-risk tumors and were predictors of poor event-free and overall survival. Conclusions: Telomere-dependent mitotic instability is present in a subgroup of WT, predominately consisting of high-risk tumors.

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Section: Discussioncontrasting

confidence: 47%

Defective Chromosome Segregation and Telomere Dysfunction in Aggressive Wilms' Tumors

Stewénius¹,

Jin²,

Øra

et al. 2007

Clinical Cancer Research

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“…Telomere shortening has been demonstrated to contribute directly to the presence of chromosomal abnormalities usually found in diverse types of cancer. This telomere reduction may trigger the formation of telomeric fusions between chromosome arms, which may result in novel karyotypic rearrangements (32,33). Different reports showed similar genetic alterations in MGUS and MM, which suggests a model for MGUS evolution based on genomic instability manifested by aneuploidy as the permissive event for the occurrence of chromosome alterations (34,35).…”

Section: Discussionmentioning

confidence: 99%

Altered mRNA Expression of Telomere-Associated Genes in Monoclonal Gammopathy of Undetermined Significance and Multiple Myeloma

Panero

Arbelbide

Fantl

et al. 2010

Mol Med

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In this study, we explored changes in the expression of the telomere maintenance genes, TRF1, TRF2 and TANK1 in patients with monoclonal gammopathy of undetermined significance (MGUS) and multiple myeloma (MM). Results were correlated with human telomerase reverse transcriptase (hTERT ) expression, telomere length (TL) and clinicopathological characteristics. Bone marrow (BM) samples from 132 patients, 64 with MGUS and 68 with MM, were studied. Real-time quantitative reverse transcription-polymerase chain reaction was used to quantify gene expression. TL was evaluated by terminal restriction fragment length analysis. MGUS patients showed increased TRF1 levels (P = 0.006) and lower expression of TRF2 (P = 0.005) and TANK1 (P = 0.003) compared with MM patients. For hTERT analysis, patients were divided into three groups by use of receiver operating characteristics: low (group I [GI]), intermediate (group II [GII]) and high (group III [GIII]) expression. We observed increasing expression of TRF2 and TANK1 from GI to GIII in MGUS and MM, with differences for both genes in MM (P < 0.01) and for TRF2 in MGUS (P < 0.01). GIII patients with the highest telomerase expression had the shortest TL. In both entities, a positive association between TRF2-TANK1, TRF2-hTERT and TANK1-hTERT (P ≤ 0.01) was observed. In MM, the percentage of BM infiltration and Ki-67 index were positively associated with TRF2, TANK1 and hTERT expression (P ≤ 0.03) and negatively with TL (P = 0.02), whereas lactate dehydrogenase was significantly correlated with TRF2 mRNA (P = 0.008). Our findings provide the first evidence of a modification in the expression of telomeric proteins in plasma cell disorders, and suggest that mechanisms other than telomerase activation are involved in TL maintenance in these pathologies.

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“…The concurrence of telomere dysfunction and centrosome amplification plays an important role in the generation of chromosomal abnormalities that are characteristically found in neoplasia, but the mechanistic link of these two distinct cellular events is still unclear. Recently, Gisselsson proposes a hypothesis that focused on this question after analysis of a series of genetic alterations in various kinds of human cancers (Gisselsson et al, 2002(Gisselsson et al, , 2004Gisselsson, 2005). According to his concept, telomeric erosion can initially induce chromosomal bridging secondary to telomeric fusion in anaphase with resultant failure in cytokinesis, giving rise to cells with supernumerary centrosomes, which consequently leads to numerical chromosomal aberrations by causing multipolar divisions.…”

Section: Discussionmentioning

confidence: 99%

Localization of TEIF in the centrosome and its functional association with centrosome amplification in DNA damage, telomere dysfunction and human cancers

et al. 2009

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Centrosomal abnormalities, multipolar mitoses, and chromosomal instability in head and neck tumours with dysfunctional telomeres

Cited by 85 publications

References 31 publications

Defective Chromosome Segregation and Telomere Dysfunction in Aggressive Wilms' Tumors

Defective Chromosome Segregation and Telomere Dysfunction in Aggressive Wilms' Tumors

Altered mRNA Expression of Telomere-Associated Genes in Monoclonal Gammopathy of Undetermined Significance and Multiple Myeloma

Localization of TEIF in the centrosome and its functional association with centrosome amplification in DNA damage, telomere dysfunction and human cancers

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