Literature DB >> 21518243

Comparative biology of mammalian telomeres: hypotheses on ancestral states and the roles of telomeres in longevity determination.

Nuno M V Gomes1, Oliver A Ryder, Marlys L Houck, Suellen J Charter, William Walker, Nicholas R Forsyth, Steven N Austad, Chris Venditti, Mark Pagel, Jerry W Shay, Woodring E Wright.   

Abstract

Progressive telomere shortening from cell division (replicative aging) provides a barrier for human tumor progression. This program is not conserved in laboratory mice, which have longer telomeres and constitutive telomerase. Wild species that do/do not use replicative aging have been reported, but the evolution of different phenotypes and a conceptual framework for understanding their uses of telomeres is lacking. We examined telomeres/telomerase in cultured cells from > 60 mammalian species to place different uses of telomeres in a broad mammalian context. Phylogeny-based statistical analysis reconstructed ancestral states. Our analysis suggested that the ancestral mammalian phenotype included short telomeres (< 20 kb, as we now see in humans) and repressed telomerase. We argue that the repressed telomerase was a response to a higher mutation load brought on by the evolution of homeothermy. With telomerase repressed, we then see the evolution of replicative aging. Telomere length inversely correlated with lifespan, while telomerase expression co-evolved with body size. Multiple independent times smaller, shorter-lived species changed to having longer telomeres and expressing telomerase. Trade-offs involving reducing the energetic/cellular costs of specific oxidative protection mechanisms (needed to protect < 20 kb telomeres in the absence of telomerase) could explain this abandonment of replicative aging. These observations provide a conceptual framework for understanding different uses of telomeres in mammals, support a role for human-like telomeres in allowing longer lifespans to evolve, demonstrate the need to include telomere length in the analysis of comparative studies of oxidative protection in the biology of aging, and identify which mammals can be used as appropriate model organisms for the study of the role of telomeres in human cancer and aging.
© 2011 The Authors. Aging Cell © 2011 Blackwell Publishing Ltd/Anatomical Society of Great Britain and Ireland.

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Year:  2011        PMID: 21518243      PMCID: PMC3387546          DOI: 10.1111/j.1474-9726.2011.00718.x

Source DB:  PubMed          Journal:  Aging Cell        ISSN: 1474-9718            Impact factor:   9.304


  49 in total

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7.  Lagomorphs (rabbits, pikas and hares) do not use telomere-directed replicative aging in vitro.

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Authors:  M Meyerson; C M Counter; E N Eaton; L W Ellisen; P Steiner; S D Caddle; L Ziaugra; R L Beijersbergen; M J Davidoff; Q Liu; S Bacchetti; D A Haber; R A Weinberg
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10.  Oxidative damage to DNA: relation to species metabolic rate and life span.

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  158 in total

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Review 3.  Genome maintenance and human longevity.

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4.  Older paternal ages and grandpaternal ages at conception predict longer telomeres in human descendants.

Authors:  Dan T A Eisenberg; Nanette R Lee; Peter H Rej; M Geoffrey Hayes; Christopher W Kuzawa
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Review 5.  Mutations, Cancer and the Telomere Length Paradox.

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Review 6.  Telomere dynamics in mice and humans.

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Review 7.  Ancestry, Telomere Length, and Atherosclerosis Risk.

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Review 8.  Mechanisms of cancer resistance in long-lived mammals.

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9.  Telomere Length is a Susceptibility Marker for Tasmanian Devil Facial Tumor Disease.

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10.  Repression of telomerase gene promoter requires human-specific genomic context and is mediated by multiple HDAC1-containing corepressor complexes.

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