François Eliaers scite author profile

Premature senescence of human diploid fibroblasts (HDFs) can be induced by exposures to a variety of oxidative stress and DNA damaging agents. In this study we developed a robust model of UVB-induced premature senescence of skin HDFs. After a series of 10 subcytotoxic (nonproapoptotic) exposures to UVB at 250 mJ/cm 2 , the socalled biomarkers of senescence were markedly expressed: growth arrest, senescence-associated β-galactosidase activity, senescence-associated gene overexpression, deletion in mitochondrial DNA. A set of 44 stress-and senescence-associated genes were found to be differentially expressed in this model, among which clusterin/ apolipoprotein J (apo J) and transforming growth factor-β1 (TGF-β1). Transfection of apo J cDNA provided protection against premature senescence-inducing doses of UVB and other stressful agents. Neutralizing antibodies against TGF-β1 or its receptor II (TβRII) sharply attenuated the senescence-associated features, suggesting a role for TGF-β1 in UVB-induced premature senescence. Both the latent and active forms of TGF-β1 were increased with time after the last UVB stress. Proteasome inhibition was ruled out as a potential mechanism of UVB-induced stress-induced premature senescence (SIPS). This model represents an alternative in vitro model in photoaging research for screening potential anti-photoaging compounds.Supplementary material available online at

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Protection of hypoxia-induced ATP decrease in endothelial cells by ginkgo beloba extract and bilobalide

Janssens

Michiels

Delaive

et al. 1995

Biochemical Pharmacology

123

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UVB-induced premature senescence of human diploid skin fibroblasts

Chainiaux

Magalhães

Eliaers

et al. 2002

The International Journal of Biochemistry & Cell Biology

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In this work, we show that repeated stresses with UVB (290-320 nm) induce stress-induced premature senescence (SIPS) of skin human diploid fibroblasts (HDFs). HDFs at early cumulative population doublings were exposed three or five times to increasing subcytotoxic doses of UVB with one stress per day. After 2 days of recovery, several biomarkers of replicative senescence were established. First, there was an increase in the proportion of cells positive for senescence-associated ␤-galactosidase activity. Second, there was a loss of replicative potential as assessed by a very low level of [ 3 H]-thymidine incorporation. Third, the steady-state level of the mRNA of three senescence-associated genes, i.e. fibronectin, osteonectin and SM22, was increased in HDFs at 72 h after three and five exposures to UVB. In conclusion, these results suggest that it is possible to induce SIPS in HDFs after repeated exposures to subcytotoxic doses of UVB. This model could be used to test whether HDFs in UVB-induced premature senescence are able to promote epithelial cell growth and tumorigenesis in skin, as shown recently with HDFs in H 2 O 2 -induced premature senescence.

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Stress-induced premature senescence and replicative senescence are different phenotypes, proteomic evidence

Dierick

Eliaers

Remacle

et al. 2002

Biochemical Pharmacology

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