2007
DOI: 10.1523/jneurosci.1139-07.2007
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Sodium Valproate Exerts Neuroprotective EffectsIn Vivothrough CREB-Binding Protein-Dependent Mechanisms But Does Not Improve Survival in an Amyotrophic Lateral Sclerosis Mouse Model

Abstract: Amyotrophic lateral sclerosis (ALS) is characterized by motoneuron (MN) degeneration, generalized weakness, and muscle atrophy. The premature death of MNs is thought to be a determinant in the onset of this disease. In a transgenic mouse model of ALS expressing the G86R mutant superoxide dismutase 1 (mSOD1), we demonstrated previously that CREB (cAMP response element-binding protein)-binding protein (CBP) and histone acetylation levels were specifically decreased in nuclei of degenerating MNs. We show here tha… Show more

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Cited by 200 publications
(150 citation statements)
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“…Sodium phenylbutyrate combined with an antioxidant [124] or riluzole [125] showed a beneficial effect. However, in the G86R mouse model, valproate restored histone acetylation in the spinal cord and CBP levels in motor neurons, but failed to improve mice survival, as a major detrimental effect on the neuromuscular junction was observed [126].…”
Section: Alsmentioning
confidence: 98%
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“…Sodium phenylbutyrate combined with an antioxidant [124] or riluzole [125] showed a beneficial effect. However, in the G86R mouse model, valproate restored histone acetylation in the spinal cord and CBP levels in motor neurons, but failed to improve mice survival, as a major detrimental effect on the neuromuscular junction was observed [126].…”
Section: Alsmentioning
confidence: 98%
“…However, an increase of p53 acetylation on K382, a known substrate for p300/CBP and HDAC SIRT1, induced apoptotic functions [138]. Thus, the CBP loss [76,126] and SIRT1 overexpression [139] observed in motor neurons might induce a neuroprotective effect.…”
Section: Alsmentioning
confidence: 99%
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“…De plus, trois études récentes ont montré que la protection du corps cellulaire du motoneurone, et donc la préserva-tion du nombre de corps cellulaires de motoneurones dans la moelle épinière, ne permettaient pas de guérir la souris SOD1m [8][9][10] : l'ablation de bax, un gène clé de l'apoptose dans le motoneurone, abolit complète-ment l'apoptose du motoneurone mais ne retarde que modestement la mort de l'animal et la dénervation musculaire [9]. De même, le valproate de sodium, qui inhibe le remodelage de la chromatine lors de l'apoptose du motoneurone, ou un inhibiteur de P38 MAPK, une protéine kinase intervenant dans les étapes initiales de l'apoptose, sont capables de protéger le corps cellulaire du motoneurone, mais ne retardent pas ou peu la dénervation musculaire et la mort de l'animal [8,10]. Comment interpréter ces résultats ?…”
Section: La Déstabilisation De La Jonction Neuromusculaire Est L'événunclassified