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Journal ArticleDOI

Telomerase: Structure, functions, and activity regulation

Maria I. Zvereva, +2 more
- 01 Dec 2010 - 
- Vol. 75, Iss: 13, pp 1563-1583
TLDR
Telomerase structure and function are summarized in this review, and they are compared for evolutionarily remote organisms and problems of telomerase activity measurement and modulation by enzyme inhibitors or activators are considered.
Abstract
Telomerase is the enzyme responsible for maintenance of the length of telomeres by addition of guanine-rich repetitive sequences. Telomerase activity is exhibited in gametes and stem and tumor cells. In human somatic cells proliferation potential is strictly limited and senescence follows approximately 50–70 cell divisions. In most tumor cells, on the contrary, replication potential is unlimited. The key role in this process of the system of the telomere length maintenance with involvement of telomerase is still poorly studied. No doubt, DNA polymerase is not capable to completely copy DNA at the very ends of chromosomes; therefore, approximately 50 nucleotides are lost during each cell cycle, which results in gradual telomere length shortening. Critically short telomeres cause senescence, following crisis, and cell death. However, in tumor cells the system of telomere length maintenance is activated. Besides catalytic telomere elongation, independent telomerase functions can be also involved in cell cycle regulation. Inhibition of the telomerase catalytic function and resulting cessation of telomere length maintenance will help in restriction of tumor cell replication potential. On the other hand, formation of temporarily active enzyme via its intracellular activation or due to stimulation of expression of telomerase components will result in telomerase activation and telomere elongation that can be used for correction of degenerative changes. Data on telomerase structure and function are summarized in this review, and they are compared for evolutionarily remote organisms. Problems of telomerase activity measurement and modulation by enzyme inhibitors or activators are considered as well.

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Citations
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Genetic etiology of oral cancer

TL;DR: This review examines, in detail, the mechanisms of genetic alteration which are considered to be responsible for the initiation of oral cancer.
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TERT promoter mutations in telomere biology.

TL;DR: Discovery of mutations within the core promoter of the TERT gene that create de novo binding sites for E-twenty-six transcription factors provided a mechanism for cancer-specific telomerase reactivation, and hold potential as biomarkers as well as future therapeutic targets.
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Telomere structure and telomerase in health and disease (review).

TL;DR: This review focuses on the structure and function of the telomere/telomerase complex and its altered behavior leading to disease, mainly cancer.
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Dual Inhibitors of Human DNA Topoisomerase II and Other Cancer-Related Targets.

TL;DR: The scientific background behind targeting topoisomerase II together with a number of other targets important in cancer therapy are discussed, the present status is reviewed and further options in the field are discussed.
Journal ArticleDOI

Telomere shortening and Alzheimer's disease.

TL;DR: It seems that there is no relationship between telomere shortening and AD, and it is essential for further clarification of telomeres-related pathogenesis in AD.
References
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Journal ArticleDOI

Identification of a specific telomere terminal transferase activity in tetrahymena extracts

TL;DR: It is proposed that the novel telomere terminal transferase is involved in the addition of telomeric repeats necessary for the replication of chromosome ends in eukaryotes.
Journal ArticleDOI

Shelterin: the protein complex that shapes and safeguards human telomeres

TL;DR: The current data argue that shelterin is emerging as a protein complex with DNA remodeling activity that acts together with several associated DNA repair factors to change the structure of the telomeric DNA, thereby protecting chromosome ends.
Journal ArticleDOI

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.
Journal ArticleDOI

The RNA component of human telomerase

TL;DR: Human cell lines that expressed hTR mutated in the template region generated the predicted mutant telomerase activity, and cells transfected with an antisense hTR lost telomeric DNA and began to die after 23 to 26 doublings.
Journal ArticleDOI

A theory of marginotomy: The incomplete copying of template margin in enzymic synthesis of polynucleotides and biological significance of the phenomenon

TL;DR: Marginotomy is responsible for the loss with age of various cell clones of the body, including some endocrine cell clones, and may be the primary cause of various disorders of age of the ageing of multicellular organisms.
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