Open Access
Open access
volume 2 pages 230-247

Stress-Induced Premature Senescence or Stress-Induced Senescence-Like Phenotype: OneIn VivoReality, Two Possible Definitions?

Olivier Toussaint 1
Patrick Dumont 2
José Remacle 1
Jean-François Dierick 1
Thierry Pascal 1
Christophe Frippiat 1
João Pedro Magalhães 1
Stephanie Zdanov 1
Florence Chainiaux 1
Publication typeJournal Article
Publication date2002-04-19
scimago Q2
SJR0.653
CiteScore5.9
Impact factor
ISSN23566140, 1537744X
PubMed ID:  12806055
General Biochemistry, Genetics and Molecular Biology
General Medicine
General Environmental Science
Abstract
No consensus exists so far on the definition of cellular senescence. The narrowest definition of senescence is irreversible growth arrest triggered by telomere shortening counting cell generations (definition 1). Other authors gave an enlarged functional definition encompassing any kind of irreversible arrest of proliferative cell types induced by damaging agents or cell cycle deregulations after overexpression of proto-oncogenes (definition 2). As stress increases, the proportion of cells in “stress-induced premature senescence-like phenotype” according to definition 1 or “stress-induced premature senescence,” according to definition 2, should increase when a culture reaches growth arrest, and the proportion of cells that reached telomere-dependent replicative senescence due to the end-replication problem should decrease. Stress-induced premature senescence-like phenotype and telomere-dependent replicatively senescent cells share basic similarities such as irreversible growth arrest and resistance to apoptosis, which may appear through different pathways. Irreversible growth arrest after exposure to oxidative stress and generation of DNA damage could be as efficient in avoiding immortalisation as “telomere-dependent” replicative senescence. Probabilities are higher that the senescent cells (according to definition 2) appearing in vivo are in stress-induced premature senescence rather than in telomere-dependent replicative senescence. Examples are given suggesting these cells affect in vivo tissue (patho)physiology and aging.
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GOST Copy
Toussaint O. et al. Stress-Induced Premature Senescence or Stress-Induced Senescence-Like Phenotype: OneIn VivoReality, Two Possible Definitions? // The Scientific World Journal. 2002. Vol. 2. pp. 230-247.
GOST all authors (up to 50) Copy
Toussaint O., Dumont P., Remacle J., Dierick J., Pascal T., Frippiat C., Magalhães J. P., Zdanov S., Chainiaux F. Stress-Induced Premature Senescence or Stress-Induced Senescence-Like Phenotype: OneIn VivoReality, Two Possible Definitions? // The Scientific World Journal. 2002. Vol. 2. pp. 230-247.
RIS |
Cite this
RIS Copy
TY - JOUR
DO - 10.1100/tsw.2002.100
UR - https://doi.org/10.1100/tsw.2002.100
TI - Stress-Induced Premature Senescence or Stress-Induced Senescence-Like Phenotype: OneIn VivoReality, Two Possible Definitions?
T2 - The Scientific World Journal
AU - Toussaint, Olivier
AU - Dumont, Patrick
AU - Remacle, José
AU - Dierick, Jean-François
AU - Pascal, Thierry
AU - Frippiat, Christophe
AU - Magalhães, João Pedro
AU - Zdanov, Stephanie
AU - Chainiaux, Florence
PY - 2002
DA - 2002/04/19
PB - Hindawi Limited
SP - 230-247
VL - 2
PMID - 12806055
SN - 2356-6140
SN - 1537-744X
ER -
BibTex
Cite this
BibTex (up to 50 authors) Copy
@article{2002_Toussaint,
author = {Olivier Toussaint and Patrick Dumont and José Remacle and Jean-François Dierick and Thierry Pascal and Christophe Frippiat and João Pedro Magalhães and Stephanie Zdanov and Florence Chainiaux},
title = {Stress-Induced Premature Senescence or Stress-Induced Senescence-Like Phenotype: OneIn VivoReality, Two Possible Definitions?},
journal = {The Scientific World Journal},
year = {2002},
volume = {2},
publisher = {Hindawi Limited},
month = {apr},
url = {https://doi.org/10.1100/tsw.2002.100},
pages = {230--247},
doi = {10.1100/tsw.2002.100}
}