Multiple cellular stressors, including activation of the tumour suppressor p53, can stimulate autophagy. Here we show that knockout, knockdown or pharmacological inhibition of p53 can induce autophagy in human, mouse and nematode cells. Enhanced autophagy improved the survival of p53-deficient cancer cells under conditions of hypoxia and nutrient depletion, allowing them to maintain high ATP levels. Inhibition of p53 led to autophagy in enucleated cells, and cytoplasmic, not nuclear, p53 was able to repress the enhanced autophagy of p53–/– cells. Many different inducers of autophagy (for example, starvation, rapamycin and toxins affecting the endoplasmic reticulum) stimulated proteasome-mediated degradation of p53 through a pathway relying on the E3 ubiquitin ligase HDM2. Inhibition of p53 degradation prevented the activation of autophagy in several cell lines, in response to several distinct stimuli. These results provide evidence of a key signalling pathway that links autophagy to the cancer-associated dysregulation of p53.

Regulation of autophagy by cytoplasmic p53 / Tasdemir, E; Maiuri, MARIA CHIARA; Galluzzi, L; Vitale, I; Djavaheri Mergny, M; D'Amelio, M; Criollo, A; Morselli, E; Zhu, C; Harper, F; Nannmark, U; Samara, C; Pinton, P; Vicencio, Jm; Carnuccio, Rosa; Moll, Um; Madeo, F; Paterlini Brechot, P; Rizzuto, R; Szabadkai, G; Pierron, G; Blomgren, K; Tavernarakis, N; Codogno, P; Cecconi, F; Kroemer, G.. - In: NATURE CELL BIOLOGY. - ISSN 1465-7392. - STAMPA. - 10:6(2008), pp. 676-687. [10.1038/ncb1730]

Regulation of autophagy by cytoplasmic p53

MAIURI, MARIA CHIARA;CARNUCCIO, ROSA;
2008

Abstract

Multiple cellular stressors, including activation of the tumour suppressor p53, can stimulate autophagy. Here we show that knockout, knockdown or pharmacological inhibition of p53 can induce autophagy in human, mouse and nematode cells. Enhanced autophagy improved the survival of p53-deficient cancer cells under conditions of hypoxia and nutrient depletion, allowing them to maintain high ATP levels. Inhibition of p53 led to autophagy in enucleated cells, and cytoplasmic, not nuclear, p53 was able to repress the enhanced autophagy of p53–/– cells. Many different inducers of autophagy (for example, starvation, rapamycin and toxins affecting the endoplasmic reticulum) stimulated proteasome-mediated degradation of p53 through a pathway relying on the E3 ubiquitin ligase HDM2. Inhibition of p53 degradation prevented the activation of autophagy in several cell lines, in response to several distinct stimuli. These results provide evidence of a key signalling pathway that links autophagy to the cancer-associated dysregulation of p53.
2008
Regulation of autophagy by cytoplasmic p53 / Tasdemir, E; Maiuri, MARIA CHIARA; Galluzzi, L; Vitale, I; Djavaheri Mergny, M; D'Amelio, M; Criollo, A; Morselli, E; Zhu, C; Harper, F; Nannmark, U; Samara, C; Pinton, P; Vicencio, Jm; Carnuccio, Rosa; Moll, Um; Madeo, F; Paterlini Brechot, P; Rizzuto, R; Szabadkai, G; Pierron, G; Blomgren, K; Tavernarakis, N; Codogno, P; Cecconi, F; Kroemer, G.. - In: NATURE CELL BIOLOGY. - ISSN 1465-7392. - STAMPA. - 10:6(2008), pp. 676-687. [10.1038/ncb1730]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11588/338006
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