Chronic treatment with calcium ionophore A23187 in NGF-differentiated cells results in cell death that is time-and concentration-dependent. Additionally, PC12 cells codifferentiated with NGF and dBcAMP become dependent on these factors for survival and undergo apoptosis when both factors are withdrawn. We show that in both cases there is a prolonged induction of c-Fos which correlates with cell death. Its continual activation in PC12 cells overexpressing c-FosER results in caspase-3 cleavage and rapid cell death. Specific phosphorylation of CREB/CREMtau transactivators or their binding to CRE of c-fos was observed. Our results indicate that prolonged c-Fos induction activates p53. There is increased nuclear localization of p53, p21 and Bax levels are induced in NGF/dBcAMP-deprived c-FosER cells, and dominant negative p53 inhibits cell death induced either by serum deprivation or by c-Fos. Overall these data implicate AP-1 as a nuclear target of signal transduction pathways which plays a role in the activation of apoptosis.
Molecular mechanisms of neuronal cell death: Implications for nuclear factors responding to cAMP and phorbol esters / S., Vyas; N. F., Biguet; Michel, Pp; Monaco, Lucia; N. S., Foulkes; G. I., Evan; P., Sassone Corsi; Y., Agid. - In: MOLECULAR AND CELLULAR NEUROSCIENCES. - ISSN 1044-7431. - STAMPA. - 21:1(2002), pp. 1-14. [10.1006/mcne.2002.1170]
Molecular mechanisms of neuronal cell death: Implications for nuclear factors responding to cAMP and phorbol esters
MONACO, Lucia;
2002
Abstract
Chronic treatment with calcium ionophore A23187 in NGF-differentiated cells results in cell death that is time-and concentration-dependent. Additionally, PC12 cells codifferentiated with NGF and dBcAMP become dependent on these factors for survival and undergo apoptosis when both factors are withdrawn. We show that in both cases there is a prolonged induction of c-Fos which correlates with cell death. Its continual activation in PC12 cells overexpressing c-FosER results in caspase-3 cleavage and rapid cell death. Specific phosphorylation of CREB/CREMtau transactivators or their binding to CRE of c-fos was observed. Our results indicate that prolonged c-Fos induction activates p53. There is increased nuclear localization of p53, p21 and Bax levels are induced in NGF/dBcAMP-deprived c-FosER cells, and dominant negative p53 inhibits cell death induced either by serum deprivation or by c-Fos. Overall these data implicate AP-1 as a nuclear target of signal transduction pathways which plays a role in the activation of apoptosis.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
