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Journal ArticleDOI

Subnuclear shuttling of human telomerase induced by transformation and DNA damage.

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TLDR
It is shown that transformation and DNA damage have opposite effects on the cellular regulation of active telomerase, affecting the enzyme's access to both telomeric and nontelomeric substrates.
Abstract
The telomerase ribonucleoprotein complex caps chromosome ends by adding telomeric repeats. Here we show that catalytically active human telomerase has a regulated intranuclear localization that is dependent on the cell-cycle stage, transformation and DNA damage. In primary cell lines, low expression of a fusion protein of green fluorescent protein and telomerase reverse transcriptase (GFP-hTERT) increases telomerase activity and stabilizes the maintenance of telomere length. Confocal microscopy shows that the release of telomerase to the nucleoplasm from sequestration at nucleolar sites is enhanced at the expected time of telomere replication. By contrast, in tumour and transformed cells, there is an almost complete dissociation of telomerase from nucleoli at all stages of the cell cycle. Transfection of the simian virus 40 genome into a primary cell line is sufficient to mobilize telomerase from nucleoli to the nucleoplasm. Conversely, ionizing radiation induces the reassociation of telomerase with nucleoli in both primary and transformed cells. These findings show that transformation and DNA damage have opposite effects on the cellular regulation of active telomerase, affecting the enzyme's access to both telomeric and nontelomeric substrates.

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Journal ArticleDOI

The multifunctional nucleolus

TL;DR: Although the nucleolus is primarily associated with ribosome biogenesis, several lines of evidence now show that it has additional functions, such as regulation of mitosis, cell-cycle progression and proliferation, many forms of stress response and biogenesis of multiple ribonucleoprotein particles.
Journal ArticleDOI

Regulation of Telomerase by Telomeric Proteins

TL;DR: The details of telomerase and its regulation by the telomere are discussed, including single-stranded DNA-binding proteins (POT1 in humans and Cdc13 in budding yeast), which have been proposed to contribute to the recruitment of telomersase and may also regulate the extent or frequency of elongation.
Journal ArticleDOI

Telomeres and telomerase: their mechanisms of action and the effects of altering their functions.

TL;DR: The molecular features of telomeres and telomerase are conserved among most eukaryotes and how they interact to promote the chromosome‐stabilizing properties of telomes are discussed here.

Telomerase maintains telomere structure in normal human cells

TL;DR: In this paper, the authors demonstrate that the rate-limiting telomerase catalytic subunit hTERT is expressed in cycling primary presenescent human fibroblasts.
Journal ArticleDOI

Telomerase maintains telomere structure in normal human cells.

TL;DR: The view that telomerase and telomere structure are dynamically regulated in normal human cells and that telomeres length alone is unlikely to trigger entry into replicative senescence is supported.
References
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Journal ArticleDOI

A survey of telomerase activity in human cancer

TL;DR: All major types of cancer have been screened and the presence of telomerase activity has been detected in the vast majority of cases, and a summary, in table form, of the current data is provided.
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Mammalian Telomeres End in a Large Duplex Loop

TL;DR: Electron microscopy reported here demonstrated that TRF2 can remodel linear telomeric DNA into large duplex loops (t loops) in vitro, which may provide a general mechanism for the protection and replication of telomeres.
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Telomere elongation in immortal human cells without detectable telomerase activity.

TL;DR: It is suggested that the presence of lengthened or stabilized telomeres is necessary for immortalization, and that this may be achieved either by the reactivation of telomerase or by a novel and as yet unidentified mechanism.
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A telomerase component is defective in the human disease dyskeratosis congenita

TL;DR: It is found that primary fibroblasts and lymphoblasts from DKC-affected males are not detectably deficient in conventional H/ACA small nucleolar RNA accumulation or function; however, DKC cells have a lower level of telomerase RNA, produce lower levels of telomersase activity and have shorter telomeres than matched normal cells.
Journal ArticleDOI

Telomeres and their control

TL;DR: This review summarizes the currently known components of the telomere/telomerase functional complex, and focuses on how they act in the control of processes occurring at telomeres.
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