Alternative lengthening of telomeres in mammalian cells

Henson, Jeremy D.; Neumann, Axel A.; Yeager, Thomas R.; Reddel, Roger R.

doi:10.1038/sj.onc.1205058

Cited by 586 publications

(501 citation statements)

References 126 publications

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“…However, telomere length maintenance can also be achieved in some tumour types in the absence of telomerase activity through an alternative recombination-based mechanism termed ALT (alternative lengthening of telomeres) (Bryan et al, 1995(Bryan et al, , 1997. Alternative lengthening of telomeres is characterised phenotypically by heterogeneous telomeres, ranging from less than 3 kb to more than 50 kb in length (Henson et al, 2002), and the presence of ALT-associated promyelocytic leukaemia (PML) bodies (APBs), which contain telomeric DNA and the telomere binding proteins, TRF1 and TRF2, in addition to several other proteins associated with DNA recombination and repair, including RAD51 and RAD52 (Yeager et al, 1999;Henson et al, 2002).…”

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“…The ALT pathway is detected in some tumours of epithelial origin, including carcinomas of the breast, lung and kidney; however, it is found at higher frequency in tumours of mesenchymal origin, such as liposarcomas, osteosarcomas and glioblastomas (Henson et al, 2002). This is thought to be due to tighter repression of telomerase expression in mesenchymal tissues, which have a slower cell turnover and less telomere shortening than many epithelial tissues (Henson et al, 2002).…”

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“…This is thought to be due to tighter repression of telomerase expression in mesenchymal tissues, which have a slower cell turnover and less telomere shortening than many epithelial tissues (Henson et al, 2002). Several studies have highlighted an association of the ALT phenotype with sarcomas that have complex karyotypes with many chromosomal losses and gains and evidence of anaphase bridge formation, more consistent with chromosomal instability, while those that have generally more simple karyotypes, including fusion genes created from chromosomal translocations, are associated with telomerase activity (Montgomery et al, 2004;Ulaner et al, 2004).…”

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High level of telomerase RNA gene expression is associated with chromatin modification, the ALT phenotype and poor prognosis in liposarcoma

et al. 2008

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Telomere length is maintained by two known mechanisms, activation of telomerase or alternative lengthening of telomeres (ALT). The ALT pathway is more commonly activated in tumours of mesenchymal origin, although the mechanisms involved in the decision of a cell to activate either telomerase or ALT are unknown at present and no molecular markers exist to define the ALT phenotype. We have previously shown an association between chromatin remodelling, telomerase gene expression and ALT in cell line models. Here, we evaluate these findings and investigate their prognostic significance in a panel of liposarcoma tissue samples to understand the biology underlying the ALT phenotype. Liposarcoma samples were split into three groups: telomerase positive (Tel þ ); ALT positive; ALTÀ/TelÀ. Differences in telomerase gene expression were evident between the groups with increased expression of hTR in ALT and Tel þ compared to ALTÀ/TelÀ samples and increased hTERT in Tel þ samples only. Investigation of a small panel of chromatin modifications revealed significantly increased binding of acetyl H3 in association with hTR expression. We confirm that the presence of the ALT phenotype is associated with poor prognosis and in addition, for the first time, we show a direct association between hTR expression and poor prognosis in liposarcoma patients.

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High level of telomerase RNA gene expression is associated with chromatin modification, the ALT phenotype and poor prognosis in liposarcoma

et al. 2008

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“…In addition to the CC assay another indicator of ALT is detection of APBs (ALT‐associated PML Bodies) (Yeager et al, 1999; Henson et al, 2002; Neumann and Reddel, 2006). We observed a significant difference between the 408 and E14 cell lines in the levels of APBs ( P = 0.0002) (Fig.…”

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Analysis of alternative lengthening of telomere markers in BRCA1 defective cells

Kargaran

Yasaei

Anjomani-Virmouni

et al. 2016

Genes Chromosomes & Cancer

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Telomeres are specialized structures responsible for the chromosome end protection. Previous studies have revealed that defective BRCA1 may lead to elevated telomere fusions and accelerated telomere shortening. In addition, BRCA1 associates with promyelocytic leukemia (PML) bodies in alternative lengthening of telomeres (ALTs) positive cells. We report here elevated recombination rates at telomeres in cells from human BRCA1 mutation carriers and in mouse embryonic stem cells lacking both copies of functional Brca1. An increased recombination rate at telomeres is one of the signs of ALT. To investigate this possibility further we employed the C‐circle assay that identifies ALT unequivocally. Our results revealed elevated levels of ALT activity in Brca1 defective mouse cells. Similar results were obtained when the same cells were assayed for the presence of another ALT marker, namely the frequency of PML bodies. These results suggest that BRCA1 may act as a repressor of ALT. © 2016 The Authors Genes, Chromosomes & Cancer Published by Wiley Periodicals, Inc.

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“…These cells acquire the capacity to maintain stable long telomeres in a telomeraseindependent manner, termed 'alternative lengthening of telomeres' or ALT (Bryan et al 1997). Some human tumors also show evidence of ALT, suggesting that ALT occurs in vivo (reviewed by Henson et al 2002). However, the mechanism(s) responsible for the ALT phenotype in human cells are not fully understood.…”

Section: Barriers To Immortalization: Crisismentioning

confidence: 99%

Immortalized cells as experimental models to study cancer

Boehm

Hahn

2004

Cytotechnology

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The development of cancer is a multi-step process in which normal cells sustain a series of genetic alterations that together program the malignant phenotype. Much of our knowledge of cancer biology results from the detailed study of specimens and cell lines derived from patient tumors. While these approaches continue to yield critical information regarding the identity, number, and types of alterations found in human tumors, further progress in understanding the molecular basis of malignant transformation depends upon the generation and use of increasingly sophisticated experimental models of cancer. Over the past several years, the recognition that telomeres and telomerase play essential roles in regulating cell lifespan now permits the development of new models of human cancer. Here we review recent progress in the use of immortalized human cells as a foundation for understanding the molecular basis of cancer.Abbreviations: ALT -alternative lengthening of telomeres; HEK -human embryonic kidney; HMEChuman mammary epithelial cell; HPV -human papillomavirus; hTERT -human telomerase reverse transcriptase; LT -SV40 Large T antigen; PD -population doubling; PP2A -protein phosphatase 2A; RalGEF -Ral guanine nucleotide exchange factor; RAS -activated H-Ras allele; shRNA -short hairpin RNA; ST -SV40 small t antigen; TRF -telomere restriction fragment.

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Alternative lengthening of telomeres in mammalian cells

Cited by 586 publications

References 126 publications

High level of telomerase RNA gene expression is associated with chromatin modification, the ALT phenotype and poor prognosis in liposarcoma

High level of telomerase RNA gene expression is associated with chromatin modification, the ALT phenotype and poor prognosis in liposarcoma

Analysis of alternative lengthening of telomere markers in BRCA1 defective cells

Immortalized cells as experimental models to study cancer

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