Telomere fusions in early human breast carcinoma

Tanaka, Hiromi; Abe, Satoshi; Huda, Nazmul; Tu, LiRen; Beam, Matthew J.; Grimes, Brenda R.; Gilley, David

doi:10.1073/pnas.1120062109

Cited by 50 publications

(66 citation statements)

References 28 publications

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“…Since we found far more frequent rate of telomere-to-telomere fusions (1.4 × 10 − 4 ), it is tempting to speculate that spontaneous chromosome fusions may be a relevant trigger of genome instability and carcinogenesis. Consistent with this idea, recent evidence show telomere-to-telomere fusions in human breast carcinoma (42). The disparity in frequencies between our result and the one previously reported may simply reflect differences in the experimental setup.…”

Section: Discussionsupporting

confidence: 57%

Spontaneous telomere to telomere fusions occur in unperturbed fission yeast cells

Almeida

Ferreira

2013

Nucleic Acids Research

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Telomeres protect eukaryotic chromosomes from illegitimate end-to-end fusions. When this function fails, dicentric chromosomes are formed, triggering breakage-fusion-bridge cycles and genome instability. How efficient is this protection mechanism in normal cells is not fully understood. We created a positive selection assay aimed at capturing chromosome-end fusions in Schizosaccharomyces pombe. We placed telomere sequences with a head to head arrangement in an intron of a selectable marker contained on a plasmid. By linearizing the plasmid between the telomere sequences, we generated a stable mini-chromosome that fails to express the reporter gene. Whenever the ends of the mini-chromosome join, the marker gene is reconstituted and fusions are captured by direct selection. Using telomerase mutants, we recovered several fusion events that lacked telomere sequences. The end-joining reaction involved specific homologous subtelomeric sequences capable of forming hairpins, suggestive of ssDNA stabilization prior to fusing. These events occurred via microhomology-mediated end-joining (MMEJ)/single-strand annealing (SSA) repair and also required MRN/Ctp1. Strikingly, we were able to capture spontaneous telomere-to-telomere fusions in unperturbed cells. Similar to disruption of the telomere regulator Taz1/TRF2, end-joining reactions occurred via non-homologous end-joining (NHEJ) repair. Thus, telomeres undergo fusions prior to becoming critically short, possibly through transient deprotection. These dysfunction events induce chromosome instability and may underlie early tumourigenesis.

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Section: Discussionsupporting

confidence: 57%

Spontaneous telomere to telomere fusions occur in unperturbed fission yeast cells

Almeida

Ferreira

2013

Nucleic Acids Research

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“…Methods to directly detect the scars of prior telomere crisis in cancer genomes have now been developed 75,149,150 . The telomere–telomere fusions that are typical of telomere crisis can be detected with a PCR-based assay that uses correctly oriented primers situated in the subtelomeric DNA of two (or more) chromosome ends 75,150 .…”

Section: Telomere Crisis and Genome Instabilitymentioning

confidence: 99%

“…The telomere–telomere fusions that are typical of telomere crisis can be detected with a PCR-based assay that uses correctly oriented primers situated in the subtelomeric DNA of two (or more) chromosome ends 75,150 . Using this approach, evidence for past telomere crisis has been obtained in CLL as well as in breast cancer, colorectal adenomas and other solid tumours 75,77,78 .…”

Section: Telomere Crisis and Genome Instabilitymentioning

confidence: 99%

Telomeres in cancer: tumour suppression and genome instability

Maciejowski

Lange

2017

Nat Rev Mol Cell Biol

523

437

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The shortening of human telomeres has two opposing effects during cancer development. On the one hand, telomere shortening can exert a tumour-suppressive effect through the proliferation arrest induced by activating the kinases ATM and ATR at unprotected chromosome ends. On the other hand, loss of telomere protection can lead to telomere crisis, which is a state of extensive genome instability that can promote cancer progression. Recent data, reviewed here, provide new evidence for the telomere tumour suppressor pathway and has revealed that telomere crisis can induce numerous cancer-relevant changes, including chromothripsis, kataegis and tetraploidization.

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“…However interstitial sequences do duplicate at termini in a rare situation, the mechanism of which is poorly understood. Two cases of direct interstitial sequences joining to telomeric sequences were described in a human cancer fusion study [140]. One was a 447 bps interstitial chromosome 4 sequence joining to 10q telomere at one side and 4p telomere at another side.…”

Section: Discussionmentioning

confidence: 99%

“…If the Telomere repeats are lost, the broken chromosome will become unstable [139][140][141], and multiple types of rearrangements can occur, including chromosome fusion [139], tips translocation [142], or direct extension of telomere repeats [141]. The manual insertion of a telomeric sequence in the interstitial region results in enhanced chromosome breakages and induces high rates of chromosome rearrangements around the insertion [143].…”

Section: Introductionmentioning

confidence: 99%

Investigation of repetitive sequences in the human genome

Shao¹

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Repetitive sequences and genomic variations mediated by repetitive sequences remain a barrier to our understanding of the function and dynamics of the human genome.Only recently have high throughput short and long reads sequencing provided an opportunity to overcome these challenges. In this thesis, I investigate the distribution, evolution and polymorphism of two types of repeats: subtelomeric and inverted repeats. I also investigate two distinct aspects of genomic mutations related to these repetitive sequences: inversion polymorphisms, and structural variation in chromosome subtelomeric regions.In the first chapter, I provide an overview of our current knowledge, as well as gaps in our understanding of the structure of the human genome. I also provide an overview of the sequencing technologies I will use in this thesis.In the second chapter, I show the performance of inversion detection by short read sequencing. Next, I develop and apply an approach for using long read nanopore sequencing data to detect inversion polymorphism. I show that using long reads it is possible to detect inversions mediated by long inverted repeats which are invisible to paired-end short read sequencing.

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Telomere fusions in early human breast carcinoma

Cited by 50 publications

References 28 publications

Spontaneous telomere to telomere fusions occur in unperturbed fission yeast cells

Spontaneous telomere to telomere fusions occur in unperturbed fission yeast cells

Telomeres in cancer: tumour suppression and genome instability

Investigation of repetitive sequences in the human genome

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