2008
DOI: 10.1074/jbc.m806432200
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Post-transcriptional Modulation of Iron Homeostasis during p53-dependent Growth Arrest

Abstract: Iron plays an essential role in cell proliferation and is a required cofactor for a number of critical cellular enzymes. In this report we investigate changes in proteins of iron metabolism during p53-mediated replicative arrest. Following the induction of p53 in H1299 lung cancer cells containing a doxycycline-inducible p53, an increase in both H and L subunits of ferritin protein was observed. To determine the mechanism of this effect, we investigated the ability of p53 to regulate ferritin. Real time revers… Show more

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Cited by 75 publications
(65 citation statements)
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“…28,29 Indeed, we show here that the protein expression of TfR1 was decreased after HZ/HNE-treatment ( Figure 7A-C,F). HZ provoked an early and irreversible loss in mean TfR1 expression on the cell surface along the whole period of ex vivo erythropoiesis, amounting to 80% expression of controls on day 1 and 75% at day 6, maintaining this low value until day 14 ( Figure 7B).…”
Section: Inhibition By Hz and Hne Of Tfr Scfr Epor Il-3r And Gatamentioning
confidence: 82%
“…28,29 Indeed, we show here that the protein expression of TfR1 was decreased after HZ/HNE-treatment ( Figure 7A-C,F). HZ provoked an early and irreversible loss in mean TfR1 expression on the cell surface along the whole period of ex vivo erythropoiesis, amounting to 80% expression of controls on day 1 and 75% at day 6, maintaining this low value until day 14 ( Figure 7B).…”
Section: Inhibition By Hz and Hne Of Tfr Scfr Epor Il-3r And Gatamentioning
confidence: 82%
“…This is why iron chelators have shown promising anti-neoplastic activity in cell cultures and clinical trials (reviewed in [52]). Interestingly, the recruitment of pathways that reduce the availability of intracellular iron is one of the mechanisms utilized by p53 to induce cell cycle arrest [53].…”
Section: Discussionmentioning
confidence: 99%
“…This is why iron chelators have shown promising anti-neoplastic activity in cell cultures and clinical trials (reviewed in [52]). Interestingly, the recruitment of pathways that reduce the availability of intracellular iron is one of the mechanisms utilized by p53 to induce cell cycle arrest [53].Circulating monocytes recruited from the circulation into the tumour differentiate into TAM, whose phenotype closely resembles that of M2 macrophages [22]. The molecular basis of the TAM functions favouring tumour growth has been related to an immunosuppressive and tumour-promoting phenotype characterized by a distinct repertoire of growth factors, cytokines, chemokines.…”
mentioning
confidence: 99%
“…Interestingly, p53 has recently been shown to contribute to growth arrest by reducing iron uptake and intracellular iron through the interaction with IRPs, 80 thus potentially providing a feed-back mechanism to control cellular iron availability.…”
Section: Discussionmentioning
confidence: 99%