Up-regulation of Caveolin Attenuates Epidermal Growth Factor Signaling in Senescent Cells

Park, Woong-Yang; Park, Jeong‐Soo; Cho, Kyung A.; Kim, Deok In; Ko, Young Gyu; Seo, Jeong Sun; Park, Sang Chul

doi:10.1074/jbc.m908162199

Cited by 209 publications

(204 citation statements)

References 41 publications

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“…Senescent cells are resistant to mitogeninduced proliferation (Aggarwal et al, 1995;Park et al, 2000), express senescence-associated b-galactosidase (SAb-gal) (Dimri et al, 1995), have a characteristic enlarged, flattened morphology (Wagner et al, 2001), and show altered gene expression (Smith and Pereira-Smith, 1996). RNA differential displays and the serial assessment of gene expression (Welle et al, 2001) have been applied to explore senescence-associated genes to gain an insight into the molecular mechanisms underlying senescence.…”

Section: Introductionmentioning

confidence: 99%

Exploration of replicative senescence-associated genes in human dermal fibroblasts by cDNA microarray technology

Yoon

Kim

et al. 2004

Experimental Gerontology

109

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Section: Introductionmentioning

confidence: 99%

Exploration of replicative senescence-associated genes in human dermal fibroblasts by cDNA microarray technology

Yoon

Kim

et al. 2004

Experimental Gerontology

109

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“…Cellular senescence has also been characterized by increases in the levels of some senescence‐associated proteins, such as P‐ERK1/2 (Lim et al ., 2000), caveolin‐1 (Park et al ., 2000), and cell cycle regulators like p53, p16 ink4a , and p21 waf1 (Yeo et al ., 2000b). Therefore, to confirm PPKO‐induced cellular senescence, we examined levels of these proteins by Western blot analysis after treating HDFs with 1 mM PPKO for 3–7 days.…”

Section: Resultsmentioning

confidence: 99%

Phenyl 2‐pyridyl ketoxime induces cellular senescence‐like alterations via nitric oxide production in human diploid fibroblasts

et al. 2015

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SummaryPhenyl‐2‐pyridyl ketoxime (PPKO) was found to be one of the small molecules enriched in the extracellular matrix of near‐senescent human diploid fibroblasts (HDFs). Treatment of young HDFs with PPKO reduced the viability of young HDFs in a dose‐ and time‐dependent manner and resulted in senescence‐associated β‐galactosidase (SA‐β‐gal) staining and G2/M cell cycle arrest. In addition, the levels of some senescence‐associated proteins, such as phosphorylated ERK1/2, caveolin‐1, p53, p16ink4a, and p21waf1, were elevated in PPKO‐treated cells. To monitor the effect of PPKO on cell stress responses, reactive oxygen species (ROS) production was examined by flow cytometry. After PPKO treatment, ROS levels transiently increased at 30 min but then returned to baseline at 60 min. The levels of some antioxidant enzymes, such as catalase, peroxiredoxin II and glutathione peroxidase I, were transiently induced by PPKO treatment. SOD II levels increased gradually, whereas the SOD I and III levels were biphasic during the experimental periods after PPKO treatment. Cellular senescence induced by PPKO was suppressed by chemical antioxidants, such as N‐acetylcysteine, 2,2,6,6‐tetramethylpiperidinyloxy, and L‐buthionine‐(S,R)‐sulfoximine. Furthermore, PPKO increased nitric oxide (NO) production via inducible NO synthase (iNOS) in HDFs. In the presence of NOS inhibitors, such as L‐NG‐nitroarginine methyl ester and L‐NG‐monomethylarginine, PPKO‐induced transient NO production and SA‐β‐gal staining were abrogated. Taken together, these results suggest that PPKO induces cellular senescence in association with transient ROS and NO production and the subsequent induction of senescence‐associated proteins.

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“…Interestingly, a close examination of the EM of caveolar structures ( Figure 6 of Bai's paper [6]), revealed that they are caveolar vesicles and not cave like structures at the membrane. These pinched off vesicles may represent a unique misregulation of caveolae in senescent cells that could explain both the functional differences and the increase in caveolar structures observed previously [7,8]. This misregulation may also explain why PTRF leads to DNA damage.…”

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confidence: 98%

“…The original investigations into the relationship between caveolae and senescence showed a unexpected upregulation of the proteins caveolin-1 and 2 during replicative senescence [7,8]. It was unclear what caused this upregulation, and now Bai et al demonstrated that it is due to the regulatory cavin protein, PTRF, which is known to drive the biogenesis of caveolae [9].…”

mentioning

confidence: 99%

“…Previous studies were at odds as to whether caveolin expression generated bona-fide functional caveolar structures [7] or represented a differential regulation of lipid rafts [8]. Interestingly, a close examination of the EM of caveolar structures ( Figure 6 of Bai's paper [6]), revealed that they are caveolar vesicles and not cave like structures at the membrane.…”

mentioning

confidence: 99%

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Caveolar vesicles generate DNA damage and perpetuate cellular aging

Wheaton

2011

Cell Res

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Up-regulation of Caveolin Attenuates Epidermal Growth Factor Signaling in Senescent Cells

Cited by 209 publications

References 41 publications

Exploration of replicative senescence-associated genes in human dermal fibroblasts by cDNA microarray technology

Exploration of replicative senescence-associated genes in human dermal fibroblasts by cDNA microarray technology

Phenyl 2‐pyridyl ketoxime induces cellular senescence‐like alterations via nitric oxide production in human diploid fibroblasts

Caveolar vesicles generate DNA damage and perpetuate cellular aging

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