Early Telomerase Inactivation Accelerates Aging Independently of Telomere Length

Artigo Acesso aberto Revisado por pares

Early Telomerase Inactivation Accelerates Aging Independently of Telomere Length

2015; Cell Press; Volume: 160; Issue: 5 Linguagem: Inglês

10.1016/j.cell.2015.02.002

ISSN

1097-4172

Autores

Zhengwei Xie, Kyle A. Jay, Dana L. Smith, Yi Zhang, Zairan Liu, Jiashun Zheng, Ruilin Tian, Hao Li, Elizabeth H. Blackburn,

Tópico(s)

DNA Repair Mechanisms

Resumo

Telomerase is required for long-term telomere maintenance and protection. Using single budding yeast mother cell analyses we found that, even early after telomerase inactivation (ETI), yeast mother cells show transient DNA damage response (DDR) episodes, stochastically altered cell-cycle dynamics, and accelerated mother cell aging. The acceleration of ETI mother cell aging was not explained by increased reactive oxygen species (ROS), Sir protein perturbation, or deprotected telomeres. ETI phenotypes occurred well before the population senescence caused late after telomerase inactivation (LTI). They were morphologically distinct from LTI senescence, were genetically uncoupled from telomere length, and were rescued by elevating dNTP pools. Our combined genetic and single-cell analyses show that, well before critical telomere shortening, telomerase is continuously required to respond to transient DNA replication stress in mother cells and that a lack of telomerase accelerates otherwise normal aging.

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Early Telomerase Inactivation Accelerates Aging Independently of Telomere Length