Abnormal synaptic protein expression and cell death in murine scrapie

Sisó, Sílvia; Puig, Berta; Varea, Ruth; Vidal, Enríc; Acín, Cristina; Prinz, Marco; Montrasio, Fabio; Badiola, J.J.; Aguzzi, Adriano; Pumarola, M.; Ferrer, Isidro

doi:10.1007/s00401-001-0512-6

Cited by 79 publications

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“…However, synaptic degeneration has been observed in multiple mouse prion disease models, 73,74 including the RML strain used for the current studies. 75 Furthermore, a decrease in SNAP25 and syntaxin has been reported in RML-infected wild-type mice. 20,75,76 Thus, contrary to the present data, synaptic transport can also be impaired in nonamyloid forms of prion disease.…”

Section: Discussionmentioning

confidence: 97%

“…75 Furthermore, a decrease in SNAP25 and syntaxin has been reported in RML-infected wild-type mice. 20,75,76 Thus, contrary to the present data, synaptic transport can also be impaired in nonamyloid forms of prion disease. The reason for this discrepancy is not clear but it is possible that decreased expression of SNARE proteins in the amyloid phenotype is the result of changes in synaptic vesicle fusion not linked to SNARE-mediated neurodegeneration, perhaps because of the lack of membrane anchored PrP C in these transgenic mice.…”

Section: Discussionmentioning

confidence: 97%

“…This hypothesis is consistent with the lack of significant gray matter spongiosis in the amyloid disease phenotype 9−11 as well as studies showing no correlation between decreased SNAP25 and apoptosis in RML infected mice. 75 …”

Section: Discussionmentioning

confidence: 99%

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Proteomics Analysis of Amyloid and Nonamyloid Prion Disease Phenotypes Reveals Both Common and Divergent Mechanisms of Neuropathogenesis

et al. 2014

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Prion diseases are a heterogeneous group of neurodegenerative disorders affecting various mammals including humans. Prion diseases are characterized by a misfolding of the host-encoded prion protein (PrPC) into a pathological isoform termed PrPSc. In wild-type mice, PrPC is attached to the plasma membrane by a glycosylphosphatidylinositol (GPI) anchor and PrPSc typically accumulates in diffuse nonamyloid deposits with gray matter spongiosis. By contrast, when mice lacking the GPI anchor are infected with the same prion inoculum, PrPSc accumulates in dense perivascular amyloid plaques with little or no gray matter spongiosis. In order to evaluate whether different host biochemical pathways were implicated in these two phenotypically distinct prion disease models, we utilized a proteomics approach. In both models, infected mice displayed evidence of a neuroinflammatory response and complement activation. Proteins involved in cell death and calcium homeostasis were also identified in both phenotypes. However, mitochondrial pathways of apoptosis were implicated only in the nonamyloid form, whereas metal binding and synaptic vesicle transport were more disrupted in the amyloid phenotype. Thus, following infection with a single prion strain, PrPC anchoring to the plasma membrane correlated not only with the type of PrPSc deposition but also with unique biochemical pathways associated with pathogenesis.

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Section: Discussionmentioning

confidence: 97%

Section: Discussionmentioning

confidence: 97%

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Proteomics Analysis of Amyloid and Nonamyloid Prion Disease Phenotypes Reveals Both Common and Divergent Mechanisms of Neuropathogenesis

et al. 2014

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“…The levels of upstream kinases DLK, MKK7, and JNK2 were also lower in scrapie-infected mice at 130 dpi, albeit only in the brainstem-cerebellum (Figure 7). The cerebellum (in the brainstem-cerebellum) may contain ~50% of all neurons in an adult mouse brain [109] and loses the most neurons in RML-infected mice, as indicated by nuclear DNA fragmentation [96]. The changes in the total levels of proteins involved in the MST1 signaling pathway in each brain region may reflect the differences in the number of affected neurons in each brain region.…”

Section: Discussionmentioning

confidence: 99%

Activation of Pro-survival CaMK4β/CREB and Pro-death MST1 signaling at early and late times during a mouse model of prion disease

Shott

Majer

Frost

et al. 2014

Virol J

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BackgroundThe signaling pathways most critical to prion disease pathogenesis are as yet incompletely characterized. We have developed a kinomics approach to identify signaling pathways that are dysregulated during prion pathogenesis. The approach is sensitive and specific enough to detect signaling pathways dysregulated in a simple in vitro model of prion pathogenesis. Here, we used this approach to identify signaling pathways dysregulated during prion pathogenesis in vivo.MethodsMice intraperitoneally infected with scrapie (strain RML) were euthanized at 70, 90, 110, 130 days post-infection (dpi) or at terminal stages of disease (155–190 dpi). The levels of 139 protein kinases in brainstem-cerebellum homogenates were analyzed by multiplex Western blots, followed by hierarchical clustering and analyses of activation states.ResultsHierarchical and functional clustering identified CaMK4β and MST1 signaling pathways as potentially dysregulated. Targeted analyses revealed that CaMK4β and its downstream substrate CREB, which promotes neuronal survival, were activated at 70 and 90 dpi in cortical, subcortical and brainstem-cerebellum homogenates from scrapie-infected mice. The activation levels of CaMK4β/CREB signaling returned to those in mock-infected mice at 110 dpi, whereas MST1, which promotes neuronal death, became activated at 130 dpi.ConclusionPro-survival CaMK4β/CREB signaling is activated in mouse scrapie at earlier times and later inhibited, whereas pro-death MST1 signaling is activated at these later times.Electronic supplementary materialThe online version of this article (doi:10.1186/1743-422X-11-160) contains supplementary material, which is available to authorized users.

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“…70 Again parallels are found between bench experiments and CJD patients, since defective synaptic machinery in infected brains (mainly (SNAP-25), syntaxin-1 and synapsin-1) was demonstrated several years ago. 27,71 However, whether these changes affect the symptoms and the evolution of the illness requires additional study. In this regard, recent approaches analyzing gene expression changes in different rodent models lacking PrP C , 18,72 and the comparison with CJD patients and prion infected animals [73][74][75][76] main problem so far resides in our lack of knowledge of the functional relevance of these interactions.…”

Section: Emerging Roles Of Prp C : Modulating Neurotransmitter Receptmentioning

confidence: 99%

Unraveling the neuroprotective mechanisms of PrP^Cin excitotoxicity

Llorens

Rı́o

2012

Prion

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Abnormal synaptic protein expression and cell death in murine scrapie

Cited by 79 publications

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Proteomics Analysis of Amyloid and Nonamyloid Prion Disease Phenotypes Reveals Both Common and Divergent Mechanisms of Neuropathogenesis

Proteomics Analysis of Amyloid and Nonamyloid Prion Disease Phenotypes Reveals Both Common and Divergent Mechanisms of Neuropathogenesis

Activation of Pro-survival CaMK4β/CREB and Pro-death MST1 signaling at early and late times during a mouse model of prion disease

Unraveling the neuroprotective mechanisms of PrP^Cin excitotoxicity

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Abnormal synaptic protein expression and cell death in murine scrapie

Cited by 79 publications

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Proteomics Analysis of Amyloid and Nonamyloid Prion Disease Phenotypes Reveals Both Common and Divergent Mechanisms of Neuropathogenesis

Proteomics Analysis of Amyloid and Nonamyloid Prion Disease Phenotypes Reveals Both Common and Divergent Mechanisms of Neuropathogenesis

Activation of Pro-survival CaMK4β/CREB and Pro-death MST1 signaling at early and late times during a mouse model of prion disease

Unraveling the neuroprotective mechanisms of PrPCin excitotoxicity

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Unraveling the neuroprotective mechanisms of PrP^Cin excitotoxicity