Mutant Prion Protein Expression Is Associated with an Alteration of the Rab GDP Dissociation Inhibitor α (GDI)/Rab11 Pathway

Massignan, Tania; Biasini, Emiliano; Lauranzano, Eliana; Veglianese, Pietro; Pignataro, Mauro; Fioriti, Luana; Salmona, Mario; Chiesa, Roberto; Bonetto, Valentina

doi:10.1074/mcp.m900271-mcp200

Cited by 34 publications

(48 citation statements)

References 56 publications

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“…Alternatively, intracellular aggregation of mutant PrP might interfere with vesicular traffic impairing delivery of essential cargo molecules to synapses. We did in fact find that D177N PrP expression in N2a cells is associated with an alteration of the GDI/Rab11 pathway governing post-Golgi vesicular traffic [66]. Finally, PG14 and D177N PrP misfolding may affect calcium homeostasis ([67] and A. Senatore and R.C.…”

Section: Discussionmentioning

confidence: 82%

Expression of Mutant or Cytosolic PrP in Transgenic Mice and Cells Is Not Associated with Endoplasmic Reticulum Stress or Proteasome Dysfunction

et al. 2011

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The cellular pathways activated by mutant prion protein (PrP) in genetic prion diseases, ultimately leading to neuronal dysfunction and degeneration, are not known. Several mutant PrPs misfold in the early secretory pathway and reside longer in the endoplasmic reticulum (ER) possibly stimulating ER stress-related pathogenic mechanisms. To investigate whether mutant PrP induced maladaptive responses, we checked key elements of the unfolded protein response (UPR) in transgenic mice, primary neurons and transfected cells expressing two different mutant PrPs. Because ER stress favors the formation of untranslocated PrP that might aggregate in the cytosol and impair proteasome function, we also measured the activity of the ubiquitin proteasome system (UPS). Molecular, biochemical and immunohistochemical analyses found no increase in the expression of UPR-regulated genes, such as Grp78/Bip, CHOP/GADD153, or ER stress-dependent splicing of the mRNA encoding the X-box-binding protein 1. No alterations in UPS activity were detected in mutant mouse brains and primary neurons using the UbG76V-GFP reporter and a new fluorogenic peptide for monitoring proteasomal proteolytic activity in vivo. Finally, there was no loss of proteasome function in neurons in which endogenous PrP was forced to accumulate in the cytosol by inhibiting cotranslational translocation. These results indicate that neither ER stress, nor perturbation of proteasome activity plays a major pathogenic role in prion diseases.

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Section: Discussionmentioning

confidence: 82%

Expression of Mutant or Cytosolic PrP in Transgenic Mice and Cells Is Not Associated with Endoplasmic Reticulum Stress or Proteasome Dysfunction

et al. 2011

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“…PrP may participate in cell signaling governing membrane protein transport (Málaga-Trillo et al., 2009) that could be altered by pathogenic mutations. We did in fact find that cells expressing D177N PrP had an impairment in Rab11-dependent trafficking (Massignan et al., 2010), which could potentially affect the endocytic recycling of α 2 δ-1 (Tran-Van-Minh and Dolphin, 2010). …”

Section: Discussionmentioning

confidence: 94%

Mutant PrP Suppresses Glutamatergic Neurotransmission in Cerebellar Granule Neurons by Impairing Membrane Delivery of VGCC α2δ-1 Subunit

Senatore

Colleoni

Verderio

et al. 2012

Neuron

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SummaryHow mutant prion protein (PrP) leads to neurological dysfunction in genetic prion diseases is unknown. Tg(PG14) mice synthesize a misfolded mutant PrP which is partially retained in the neuronal endoplasmic reticulum (ER). As these mice age, they develop ataxia and massive degeneration of cerebellar granule neurons (CGNs). Here, we report that motor behavioral deficits in Tg(PG14) mice emerge before neurodegeneration and are associated with defective glutamate exocytosis from granule neurons due to impaired calcium dynamics. We found that mutant PrP interacts with the voltage-gated calcium channel α2δ-1 subunit, which promotes the anterograde trafficking of the channel. Owing to ER retention of mutant PrP, α2δ-1 accumulates intracellularly, impairing delivery of the channel complex to the cell surface. Thus, mutant PrP disrupts cerebellar glutamatergic neurotransmission by reducing the number of functional channels in CGNs. These results link intracellular PrP retention to synaptic dysfunction, indicating new modalities of neurotoxicity and potential therapeutic strategies.

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“…Few proteomics studies have been made in cultured cells for investigating molecular pathogenesis of prion disorders. [5][6][7][8] Proteomic differential protein expression analysis represents however an interesting approach that could complete previous genomic studies. [9][10][11][12] In this article we performed a proteomic investigation in an integrated cellular model where both differential PrP C expression and conversion could be obtained.…”

Section: Proteomic Consequences Of Expression and Pathological Convermentioning

confidence: 99%

Proteomic consequences of expression and pathological conversion of the prion protein in inducible neuroblastoma N2a cells

Provansal

Roche

Pastore

et al. 2010

Prion

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Neurodegenerative diseases are often associated with misfolding and deposition of specific proteins in the nervous system. The prion protein, which is associated with transmissible spongiform encephalopathies (TSEs), is one of them. The normal function of the cellular form of the prion protein (PrP(C)) is mediated through specific signal transduction pathways and is linked to resistance to oxidative stress, neuronal outgrowth and cell survival. In TSEs, PrP(C) is converted into an abnormally folded isoform, called PrP(Sc), that may impair the normal function of the protein and/or generate toxic aggregates. To investigate these molecular events we performed a two-dimensional gel electrophoresis comparison of neuroblastoma N2a cells expressing different amounts of PrP(C) and eventually infected with the 22L prion strain. Mass spectrometry and peptide mass fingerprint analysis identified a series of proteins with modified expression. They included the chaperones Grp78/BiP, protein disulfide-isomerase A6, Grp75 and Hsp60 which had an opposite expression upon PrPC expression and PrP(Sc) production. The detection of these proteins was coherent with the idea that protein misfolding plays an important role in TSEs. Other proteins, such as calreticulin, tubulin, vimentin or the laminin receptor had their expression modified in infected cells, which was reminiscent of previous results. Altogether our data provide molecular information linking PrP expression and misfolding, which could be the basis of further therapeutic and pathophysiological research in this field.

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Mutant Prion Protein Expression Is Associated with an Alteration of the Rab GDP Dissociation Inhibitor α (GDI)/Rab11 Pathway

Cited by 34 publications

References 56 publications

Expression of Mutant or Cytosolic PrP in Transgenic Mice and Cells Is Not Associated with Endoplasmic Reticulum Stress or Proteasome Dysfunction

Expression of Mutant or Cytosolic PrP in Transgenic Mice and Cells Is Not Associated with Endoplasmic Reticulum Stress or Proteasome Dysfunction

Mutant PrP Suppresses Glutamatergic Neurotransmission in Cerebellar Granule Neurons by Impairing Membrane Delivery of VGCC α2δ-1 Subunit

Proteomic consequences of expression and pathological conversion of the prion protein in inducible neuroblastoma N2a cells

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