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Journal ArticleDOI

The load of short telomeres, estimated by a new method, Universal STELA, correlates with number of senescent cells

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TLDR
This new method, Universal STELA, offers some advantages compared to existing methods and can be used to explore many of the unanswered questions in telomere biology including the role that telomeres play in cancer and aging.
Abstract
Short telomeres are thought to trigger senescence, most likely through a single - or a group of few - critically shortened telomeres. Such short telomeres are thought to result from a combination of gradual linear shortening resulting from the end replication problem, reflecting the division history of the cell, superimposed by a more stochastic mechanism, suddenly causing a significant shortening of a single telomere. Previously, studies that have tried to explore the role of critically shortened telomeres have been hampered by methodological problems. With the method presented here, Universal STELA, we have a tool that can directly investigate the relationship between senescence and the load of short telomeres. The method is a variant of the chromosome-specific STELA method but has the advantage that it can demonstrate short telomeres regardless of chromosome. With Universal STELA, we find a strong correlation between the load of short telomeres and cellular senescence. Further we show that the load of short telomeres is higher in senescent cells compared to proliferating cells at the same passage, offering an explanation of premature cell senescence. This new method, Universal STELA, offers some advantages compared to existing methods and can be used to explore many of the unanswered questions in telomere biology including the role that telomeres play in cancer and aging.

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Journal ArticleDOI

Telomere Length in Epidemiology: A Biomarker of Aging, Age-Related Disease, Both, or Neither?

TL;DR: It is demonstrated that shorter LTL is associated with older age, male gender, Caucasian race, and possibly atherosclerosis; associations with other markers of health are equivocal.
Journal ArticleDOI

Telomeres and telomerase: three decades of progress.

TL;DR: This Timeline article highlights the key advances that have expanded the views on the mechanistic underpinnings of telomeres and telomerase and their roles in ageing and disease.
Journal ArticleDOI

Role of Telomeres and Telomerase in Aging and Cancer

TL;DR: This review focuses on the current state of advances in the telomerase area, identifies outstanding questions, and addresses areas and methods that need refinement and how recent advances could affect future research and treatment approaches.
Journal ArticleDOI

Measurement of telomere length by the Southern blot analysis of terminal restriction fragment lengths

TL;DR: A method to obtain telomere length parameters using Southern blots of terminal restriction fragments (TRFs) is described, which requires a considerable amount of DNA and measures both the canonical and noncanonical components of telomeres.
Journal ArticleDOI

Is Telomere Length a Biomarker of Aging? A Review

TL;DR: The evidence suggesting telomere length is a biomarker of aging in humans is equivocal and more studies examining the relationships between telomeres length and mortality and with measures that decline with "normal" aging in community samples are required.
References
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Journal ArticleDOI

Telomeres shorten during ageing of human fibroblasts.

TL;DR: The amount and length of telomeric DNA in human fibroblasts does in fact decrease as a function of serial passage during ageing in vitro and possibly in vivo.
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Extension of life-span by introduction of telomerase into normal human cells

TL;DR: In this article, two telomerase-negative normal human cell types, retinal pigment epithelial cells and foreskin fibroblasts, were transfected with vectors encoding the human telomere catalytic subunit.
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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.
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A DNA damage checkpoint response in telomere-initiated senescence

TL;DR: It is proposed that telomere-initiated senescence reflects a DNA damage checkpoint response that is activated with a direct contribution from dysfunctional telomeres.
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Universal and rapid salt-extraction of high quality genomic DNA for PCR-based techniques

TL;DR: The quantity and the quality of the DNA extracted by this method is high enough to perform hundreds of PCR-based reactions and also to be used in other DNA manipulation techniques such as restriction digestion, Southern blot and cloning.
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