Neuroprotective effects of pituitary adenylate cyclase–activating polypeptide (PACAP) in MPP+‐induced alteration of translational control in Neuro‐2a neuroblastoma cells
Identifieur interne : 000117 ( France/Analysis ); précédent : 000116; suivant : 000118Neuroprotective effects of pituitary adenylate cyclase–activating polypeptide (PACAP) in MPP+‐induced alteration of translational control in Neuro‐2a neuroblastoma cells
Auteurs : Julie Deguil [France] ; David Jailloux [France] ; Guylène Page [France] ; Bernard Fauconneau [France] ; Jean-Luc Houeto [France] ; Michel Philippe [France] ; Jean-Marc Muller [France] ; Stéphanie Pain [France]Source :
- Journal of Neuroscience Research [ 0360-4012 ] ; 2007-07.
English descriptors
Abstract
Parkinson's disease (PD) and 1‐methyl‐4‐phenyl‐1,2,3,6‐tetrahydropyridine (MPTP) toxicity are both associated with dopaminergic neuron death in the substantia nigra. Although a variety of evidence has shown that degenerative cells have apoptotic features, the role of apoptosis in disease pathology remains controversial. The 1‐methyl‐4‐phenylpyridinium ion (MPP+), a metabolite of MPTP, was recently shown to alter the expression of proteins involved in translational control. The initiation step of translational control is regulated by a cascade of phosphorylation affecting proteins of the antiapoptotic way controlled by mammalian target of rapamycin (mTOR) and of the proapoptotic way controlled by double‐stranded RNA protein–dependent kinase (PKR). A study showed that MPP+ induced an increase in eIF2α phosphorylation, leading to inhibition of protein synthesis. The aims of our study were: (1) to assess the effects of MPP+ toxicity on molecular factors of PKR and mTOR signaling pathways in murine neuroblastoma cells, and (2) to examine the ability of VIP and PACAP peptides to counteract the MPP+ toxicity. Our findings showed that MPP+ induced phosphorylation of eIF2α and significantly reduced the expression of phosphorylated mTOR, p70S6K, eIF4E, and 4E‐BP1, suggesting its toxicity in controlling protein synthesis. Furthermore, the VIP peptide had no effect on either the PKR or the mTOR signaling pathway. On the contrary, the PACAP 27 neuropeptide prevented MPP+‐induced eIF2α phosphorylation and blocked MPP+ toxicity in molecular factors of the mTOR pathway. And last, PACAP 27 seemed to protect Neuro‐2a cells from the apoptotic process as assessed by the decreased nuclear condensation after DAPI staining. These results could open new paths of research of PACAP in PD. © 2007 Wiley‐Liss, Inc.
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DOI: 10.1002/jnr.21318
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Although a variety of evidence has shown that degenerative cells have apoptotic features, the role of apoptosis in disease pathology remains controversial. The 1‐methyl‐4‐phenylpyridinium ion (MPP+), a metabolite of MPTP, was recently shown to alter the expression of proteins involved in translational control. The initiation step of translational control is regulated by a cascade of phosphorylation affecting proteins of the antiapoptotic way controlled by mammalian target of rapamycin (mTOR) and of the proapoptotic way controlled by double‐stranded RNA protein–dependent kinase (PKR). A study showed that MPP+ induced an increase in eIF2α phosphorylation, leading to inhibition of protein synthesis. The aims of our study were: (1) to assess the effects of MPP+ toxicity on molecular factors of PKR and mTOR signaling pathways in murine neuroblastoma cells, and (2) to examine the ability of VIP and PACAP peptides to counteract the MPP+ toxicity. Our findings showed that MPP+ induced phosphorylation of eIF2α and significantly reduced the expression of phosphorylated mTOR, p70S6K, eIF4E, and 4E‐BP1, suggesting its toxicity in controlling protein synthesis. Furthermore, the VIP peptide had no effect on either the PKR or the mTOR signaling pathway. On the contrary, the PACAP 27 neuropeptide prevented MPP+‐induced eIF2α phosphorylation and blocked MPP+ toxicity in molecular factors of the mTOR pathway. And last, PACAP 27 seemed to protect Neuro‐2a cells from the apoptotic process as assessed by the decreased nuclear condensation after DAPI staining. These results could open new paths of research of PACAP in PD. © 2007 Wiley‐Liss, Inc.</div></front></TEI><affiliations><list><country><li>France</li></country><settlement><li>Poitiers</li></settlement></list><tree><country name="France"><noRegion><name sortKey="Deguil, Julie" sort="Deguil, Julie" uniqKey="Deguil J" first="Julie" last="Deguil">Julie Deguil</name></noRegion><name sortKey="Fauconneau, Bernard" sort="Fauconneau, Bernard" uniqKey="Fauconneau B" first="Bernard" last="Fauconneau">Bernard Fauconneau</name><name sortKey="Fauconneau, Bernard" sort="Fauconneau, Bernard" uniqKey="Fauconneau B" first="Bernard" last="Fauconneau">Bernard Fauconneau</name><name sortKey="Houeto, Jean Uc" sort="Houeto, Jean Uc" uniqKey="Houeto J" first="Jean-Luc" last="Houeto">Jean-Luc Houeto</name><name sortKey="Houeto, Jean Uc" sort="Houeto, Jean Uc" uniqKey="Houeto J" first="Jean-Luc" last="Houeto">Jean-Luc Houeto</name><name sortKey="Jailloux, David" sort="Jailloux, David" uniqKey="Jailloux D" first="David" last="Jailloux">David Jailloux</name><name sortKey="Muller, Jean Arc" sort="Muller, Jean Arc" uniqKey="Muller J" first="Jean-Marc" last="Muller">Jean-Marc Muller</name><name sortKey="Page, Guylene" sort="Page, Guylene" uniqKey="Page G" first="Guylène" last="Page">Guylène Page</name><name sortKey="Pain, Stephanie" sort="Pain, Stephanie" uniqKey="Pain S" first="Stéphanie" last="Pain">Stéphanie Pain</name><name sortKey="Pain, Stephanie" sort="Pain, Stephanie" uniqKey="Pain S" first="Stéphanie" last="Pain">Stéphanie Pain</name><name sortKey="Philippe, Michel" sort="Philippe, Michel" uniqKey="Philippe M" first="Michel" last="Philippe">Michel Philippe</name></country></tree></affiliations></record>Pour manipuler ce document sous Unix (Dilib)
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