Constitutive telomerase expression promotes mammary carcinomas in aging mice

Artandi, Maja; Alson, Scott; Tietze, Maja Katrin; Sharpless, Norman E.; Ye, Siqin; Greenberg, Roger A.; Castrillón, Diego H.; Horner, James W.; Weiler, Sarah R.; Carrasco, Ruben D.; DePinho, Ronald A.

doi:10.1073/pnas.112515399

Cited by 284 publications

(185 citation statements)

References 37 publications

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“…Recent data support the emerging idea that hTERT/telomerase possesses pro-tumorigenic activities that extend beyond its classical role in telomere elongation. Interestingly, in mouse tumours originating from telomerasepositive tissues, an increase in telomerase activity has been observed, and overexpression of telomerase supports tumour formation in mouse tissues with long telomeres, indicating that telomerase has functions in tumorigenesis that are independent of telomere lengthening 1,[26][27][28] .…”

Section: Discussionmentioning

confidence: 99%

Telomerase stimulates ribosomal DNA transcription under hyperproliferative conditions

et al. 2014

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In addition to performing its canonical function, Telomerase Reverse Transcriptase (TERT) has been shown to participate in cellular processes independent of telomerase activity. Furthermore, although TERT mainly localizes to Cajal bodies, it is also present within the nucleolus. Because the nucleolus is the site of rDNA transcription, we investigated the possible role of telomerase in regulating RNA polymerase I (Pol I). Here we show that TERT binds to rDNA and stimulates transcription by Pol I during liver regeneration and Ras-induced hyperproliferation. Moreover, the inhibition of telomerase activity by TERT-or TERC-specific RNA interference, the overexpression of dominant-negative-TERT, and the application of the telomerase inhibitor imetelstat reduce Pol I transcription and the growth of tumour cells. In vitro, telomerase can stimulate the formation of the transcription initiation complex. Our results demonstrate how non-canonical features of telomerase may direct Pol I transcription in oncogenic and regenerative hyperproliferation.

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Section: Discussionmentioning

confidence: 99%

Telomerase stimulates ribosomal DNA transcription under hyperproliferative conditions

et al. 2014

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“…Both in vitro and in vivo, overexpression of telomerase in cancer cells appears to be crucial for tumor progression (Greenberg et al, 1999;Hahn et al, 1999a, b;Gonzalez-Suarez et al, 2000Elenbaas et al, 2001;Artandi et al, 2002). On the other hand, studies on mice lacking the telomerase RNA gene demonstrate that critical telomere shortening and telomere instability can favor initial stages of cancer formation and cooperates with p53 deficiency to favor carcinogenesis Rudolph et al, 2001).…”

Section: Introductionmentioning

confidence: 99%

TRF2 inhibition promotes anchorage-independent growth of telomerase-positive human fibroblasts

et al. 2005

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Although telomere instability is observed in human tumors and is associated with the development of cancers in mice, it has yet to be established that it can contribute to the malignant transformation of human cells. We show here that in checkpoint-compromised telomerase-positive human fibroblasts an episode of TRF2 inhibition promotes heritable changes that increase the ability to grow in soft agar, but not tumor growth in nude mice. This transforming activity is associated to a burst of telomere instability but is independent of an altered control of telomere length. Moreover, it cannot be recapitulated by an increase in chromosome breaks induced by an exposure to cradiations. Since it can be revealed in the context of telomerase-proficient human cells, telomere dysfunction might contribute to cancer progression even at late stages of the oncogenesis process, after the telomerase reactivation step.

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“…Over the last few years, it has become clear that telomere shortening is probably a minor factor in the initiation of genomic instability, although telomerase reactivation probably plays an important role in tumor progression. 28 DNA repair defects 29 or fragile sites 30 have alternatively been suggested to initiate genetic instability. In contrast to a proposed repair defect, many CIN tumors show upregulation of DSB repair pathways such as non-homologous end joining.…”

Section: Are Aneuploidy and Chromosome Breakage Caused By A Cingle Mementioning

confidence: 99%

Are aneuploidy and chromosome breakage caused by a CINgle mechanism?

Martı́nez-A

Wely

2010

Cell Cycle

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G enetic instability is a hallmark of cancer. Most tumors show complex patterns of translocations, amplifications and deletions, which have occupied scientists for decades. A specific problem arises in carcinomas with a genetic defect termed chromosomal instability; these solid tumors undergo gains and losses of entire chromosomes, as well as segmental defects caused by chromosome breaks. To date, the apparent inconsistency between intact and broken chromosomes has precluded identification of an underlying mechanism. The recent identification of centromeric breaks alongside aneuploidy in cells with spindle defects indicates that a single mechanism could account for all genetic alterations characteristic of chromosomal instability. Since a poorly controlled spindle can cause merotelic attachments, kinetochore distortion and subsequent chromosome breakage, spindle defects can generate the sticky ends necessary to start a breakagefusion-bridge cycle. The characteristic breakpoint of spindle-generated damage, adjacent to the centromere, also explains the losses and gains of whole chromosome arms, which are especially prominent in low-grade tumors. The recent data indicate that spindle defects are an early event in tumor formation, and an important initiator of carcinogenesis.

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Constitutive telomerase expression promotes mammary carcinomas in aging mice

Cited by 284 publications

References 37 publications

Telomerase stimulates ribosomal DNA transcription under hyperproliferative conditions

Telomerase stimulates ribosomal DNA transcription under hyperproliferative conditions

TRF2 inhibition promotes anchorage-independent growth of telomerase-positive human fibroblasts

Are aneuploidy and chromosome breakage caused by a CINgle mechanism?

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