Altered Neuron Excitability and Synaptic Plasticity in the Cerebellar Granular Layer of Juvenile Prion Protein Knock-Out Mice with Impaired Motor Control

Prestori, Francesca; Rossi, Paola; Bearzatto, Bertrand; Lainé, Jeanne; Necchi, Daniela; Diwakar, Shyam; Schiffmann, Serge N.; Axelrad, H.; D’Angelo, Egidio

doi:10.1523/jneurosci.0409-08.2008

Cited by 71 publications

(73 citation statements)

References 77 publications

(103 reference statements)

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“…In the context of our study it is noteworthy that differentiation of granule cells and cerebellar network formation is retarded in PrP-deficient mice, confirming the role of PrP in brain development (Prestori et al, 2008). In our present study, the potentiating effect of PrP on inhibition of neurite outgrowth was tested not only in vitro but also in vivo; in agreement with our in vitro data, constitutive absence of PrP in mice leads to enhanced regeneration after spinal cord injury in terms of recovery of locomotor functions and regrowth of serotonergic and adrenergic axons into the caudal part of the lesioned spinal cord of adult mice.…”

Section: Discussionsupporting

confidence: 84%

Cellular Form of Prion Protein Inhibits Reelin-Mediated Shedding of Caspr from the Neuronal Cell Surface to Potentiate Caspr-Mediated Inhibition of Neurite Outgrowth

Devanathan

Jakovčevski

Santuccione

et al. 2010

Journal of Neuroscience

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Extension of axonal and dendritic processes in the CNS is tightly regulated by outgrowth-promoting and -inhibitory cues to assure precision of synaptic connections. We identify a novel role for contactin-associated protein (Caspr) as an inhibitory cue that reduces neurite outgrowth from CNS neurons. We show that proteolysis of Caspr at the cell surface is regulated by the cellular form of prion protein (PrP), which directly binds to Caspr. PrP inhibits Reelin-mediated shedding of Caspr from the cell surface, thereby increasing surface levels of Caspr and potentiating the inhibitory effect of Caspr on neurite outgrowth. PrP deficiency results in reduced levels of Caspr at the cell surface, enhanced neurite outgrowth in vitro, and more efficient regeneration of axons in vivo following spinal cord injury. Thus, we reveal a previously unrecognized role for Caspr and PrP in inhibitory modulation of neurite outgrowth in CNS neurons, which is counterbalanced by the proteolytic activity of Reelin.

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Section: Discussionsupporting

confidence: 84%

Cellular Form of Prion Protein Inhibits Reelin-Mediated Shedding of Caspr from the Neuronal Cell Surface to Potentiate Caspr-Mediated Inhibition of Neurite Outgrowth

Devanathan

Jakovčevski

Santuccione

et al. 2010

Journal of Neuroscience

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“…Also in agreement with our results is the demonstration that the absence of PrP C protracted both mitosis of cerebellar granule cell precursors and maturation of the granule layer in the first post-natal weeks, and that both events did not compromise the final acquisition of a normal architecture of the cerebellum. 25 Thus, all these findings support the contention that, by affecting the rate, but not the end point, of tissue morphogenesis, PrP C is involved in the maturation of different tissues. As our data have highlighted the importance of using in vivo models to best decipher the physiologic action of PrP C , this same mean of experimentation could be used to…”

Section: Prp C As Regulator Of Extracellular Matrix Proteasessupporting

confidence: 69%

Prion and TNFα: TAC(E)it agreement between the prion protein and cell signaling

Stella

Massimino²,

Sorgato

et al. 2010

Cell Cycle

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“…The latter notion is consistent with the delayed maturation of different types of PrP C -less neurons, observed both in vitro and in vivo. 32,33 If one assumes that the interaction of PrP C with multiple partners (45 for PrP C and PrP Sc , as reviewed in Aguzzi et al, 5 or 46 considering the homophylic interaction) are all functionally significant, the most immediate interpretation of this "sticky" behavior entails that PrP C acts as a scaffolding protein in different membrane protein complexes. 5,6 Each complex could then activate a specific signaling pathway depending on the type and maturation of cells, the expression and glycosylation of PrP C , and availability of extra-and intra-cellular signaling partners.…”

mentioning

confidence: 99%