Preventing polyglutamine-induced activation of c-Jun delays neuronal dysfunction in a mouse model of SCA7 retinopathy

Mérienne, Karine; Friedman, James S.; Akimoto, Masayuki; Abou-Sleymane, Gretta; Weber, C. R.; Swaroop, Anand; Trottier, Yvon

doi:10.1016/j.nbd.2006.11.002

Cited by 14 publications

(14 citation statements)

References 68 publications

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“…Retinal ischemia induced by elevation of intraocular pressure leads to activation of JNK and p38 MAP kinases within the first 6 h (Roth et al 2003;Merienne et al 2007;Roduit and Schorderet 2008). Long-term activation of MAP kinases has also been reported in excitotoxic retinal damage, with activation beginning 1-6 h after the NMDA treatment or the ischemic insult (Zhang et al 2002;Munemasa et al 2005).…”

Section: Discussionmentioning

confidence: 99%

“…Another group of rats underwent the same surgical procedure for bilateral carotid occlusion (n = 9) or sham operation (n = 5) and retinas were removed after 4 h in order to investigate the signaling pathways that are activated within the first few hours after an ischemic insult (Roth et al 2003;Merienne et al 2007;Roduit and Schorderet 2008). Samples were processed for Western blot analysis as described earlier (Racz et al 2007).…”

Section: Western Blotmentioning

confidence: 99%

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Protection Against Chronic Hypoperfusion-Induced Retinal Neurodegeneration by PARP Inhibition via Activation of PI-3-kinase Akt Pathway and Suppression of JNK and p38 MAP Kinases

et al. 2009

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Poly(ADP-ribose) polymerase (PARP) activation is considered as a major regulator of cell death in various pathophysiological conditions, however, no direct information is available about its role in chronic hypoperfusion-induced neuronal death. Here, we provide evidence for the protective effect of PARP inhibition on degenerative retinal damage induced by bilateral common carotid artery occlusion (BCCAO), an adequate chronic hypoperfusion murine model. We found that BCCAO in adult male Wistar rats led to severe degeneration of all retinal layers that was attenuated by a carboxaminobenzimidazol-derivative PARP inhibitor (HO3089) administered unilaterally into the vitreous body immediately following carotid occlusion and then 4 times in a 2-week-period. Normal morphological structure of the retina was preserved and the thickness of the retinal layers was increased in HO3089-treated eyes compared to the BCCAO eyes. For Western blot studies, HO3089 was administered immediately after BCCAO and retinas were removed 4 h later. According to Western blot analysis utilizing phosphorylation-specific primary antibodies, besides activating poly-ADP-ribose (PAR) synthesis, BCCAO induced phosphorylation of c-Jun N-terminal kinase (JNK) and p38 mitogen-activated protein kinase (MAPK). HO3089 inhibited PAR synthesis, and decreased the phosphorylation of these proapoptotic MAPKs. In addition, HO3089 treatment induced phosphorylation, that is activation, of the protective Akt/glycogen synthase kinase (GSK)-3beta and extracellular signal-regulated kinase (ERK1/2) signaling pathways. These data indicate that PARP activation has a major role in mediating chronic hypoperfusion-induced neuronal death, and inhibition of the enzyme prevents the pathological changes both in the morphology and the kinase signaling cascades involved. These results identify PARP inhibition as a possible molecular target in the clinical management of chronic hypoperfusion-induced neurodegenerative diseases including ocular ischemic syndrome.

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Section: Discussionmentioning

confidence: 99%

Section: Western Blotmentioning

confidence: 99%

Protection Against Chronic Hypoperfusion-Induced Retinal Neurodegeneration by PARP Inhibition via Activation of PI-3-kinase Akt Pathway and Suppression of JNK and p38 MAP Kinases

et al. 2009

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“…R7E transgenic mice develop a phenotype earlier than P7E mice, with a pathology that includes NIIs formation, retinal photoreceptor dysfunction, and neurodegeneration (Helmlinger et al, 2004aYefimova et al, 2010;Yvert et al, 2000). Notably, the deactivation of the JNK/c-Jun stress pathway in R7E mice ameliorates retinopathy and may be a promising finding for future therapies (Merienne et al, 2007). In the R7E mouse retina, mutant ataxin-7 alters the recruitment of the SAGA complex to chromatin resulting in H3 hyperacetylation, leading to transcriptional deregulation of rod differentiation and retinopathy .…”

Section: Cell-specific Sca7 Models With Pcp2 (L7) Rhodopsin and Gfamentioning

confidence: 99%

“…Among other therapeutic strategies under investigation for polyQ ataxias are modulation of signal transduction pathways (Merienne et al, 2007), induction of neuroprotective effects with growth factors or stem cell transplantation (Chang et al, 2011a,b;Noma et al, 2012), and modulation of calpain activity (Simões et al, 2012).…”

Section: Therapies For Polyq Diseasesmentioning

confidence: 99%

Mouse Models of SCA3 and Other Polyglutamine Repeat Ataxias

et al. 2015

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“…Expression-analysis revealed that nearly all rod-specific genes were affected, leading to visual impairment in SCA7 mice. When these mice were crossed with a knock-in line expressing JUNAA, an alanine-substituted form of jun which is inactive, the retinal phenotype was improved and there was restoration of Nrl, a factor active in transcription of rod-specific proteins [62]. …”

Section: Sca7mentioning

confidence: 99%

Genetically engineered mouse models of the trinucleotide-repeat spinocerebellar ataxias

Ingram

Orr

Clark

2012

Brain Research Bulletin

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The spinocerebellar ataxias (SCA) are dominantly inherited disorders that primarily affect coordination of motor function but also frequently involve other brain functions. The models described in this review address mechanisms of trinucleotide-repeat expansions, particularly those relating to polyglutamine expression in the mutant proteins. Modeling chronic late-onset human ataxias in mice is difficult because of their short life-span. While this potential hindrance has been partially overcome by using over-expression of the mutant gene, and/or worsening of the mutation by increasing the length of the trinucleotide repeat expansion, interpretation of results from such models and extrapolation to the human condition should be cautious. Nevertheless, genetically engineered murine models of these diseases have enhanced our understanding of the pathogenesis of many of these conditions. A common theme in many of the polyglutamine-repeat diseases is nuclear localization of mutant protein, with resultant effects on gene regulation. Conditional mutant models and transgenic knock-down therapy have demonstrated the potential for reversibility of disease when production of mutant protein is halted. Several other genetically engineered murine models of SCA also have begun to show utility in the identification and assessment of more classical drug-based therapeutic modalities.

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Preventing polyglutamine-induced activation of c-Jun delays neuronal dysfunction in a mouse model of SCA7 retinopathy

Cited by 14 publications

References 68 publications

Protection Against Chronic Hypoperfusion-Induced Retinal Neurodegeneration by PARP Inhibition via Activation of PI-3-kinase Akt Pathway and Suppression of JNK and p38 MAP Kinases

Protection Against Chronic Hypoperfusion-Induced Retinal Neurodegeneration by PARP Inhibition via Activation of PI-3-kinase Akt Pathway and Suppression of JNK and p38 MAP Kinases

Mouse Models of SCA3 and Other Polyglutamine Repeat Ataxias

Genetically engineered mouse models of the trinucleotide-repeat spinocerebellar ataxias

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