Nucleation-Dependent Polymerization Is an Essential Component of Amyloid-Mediated Neuronal Cell Death

Wogulis, Mark; Wright, Sarah; Cunningham, Damian F.; Chilcote, Tamie J.; Powell, Kyle; Rydel, Russell E.

doi:10.1523/jneurosci.2381-04.2005

Cited by 209 publications

(186 citation statements)

References 46 publications

(64 reference statements)

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“…Similarly, using SEC-isolated Aβ42 protofibrils, we have shown that monomeric Aβ40 inhibited Aβ42 protofibril toxicity toward cultured neurons by altering their aggregation properties and inhibiting fibril formation. These observations reinforced the importance of an ongoing Aβ-nucleated polymerization as a critical factor for Aβ-induced toxicity 21,66 .…”

Section: High Molecular Weightsupporting

confidence: 62%

Preparation and characterization of toxic Aβ aggregates for structural and functional studies in Alzheimer's disease research

2010

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Section: High Molecular Weightsupporting

confidence: 62%

Preparation and characterization of toxic Aβ aggregates for structural and functional studies in Alzheimer's disease research

2010

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“…The different behavior of A-oligomers (non-toxic) with respect to A+ oligomers (toxic) was confirmed in human SH-SY5Y neuroblastoma cells by using the MTT assay (Fig. 1B), taking into account some concerns regarding a nonspecific interference of A␤ peptide with MTT reduction [54]. However, A-oligomers become significantly toxic in cells enriched in GM1 content by a factor of ca.…”

Section: Harmless Aβ 42 Oligomers Become Toxic In Gm1-enriched Neuronmentioning

confidence: 71%

Soluble Oligomers Require a Ganglioside to Trigger Neuronal Calcium Overload

Cascella

Evangelisti

Bigi

et al. 2017

JAD

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Abstract. An altered distribution of membrane gangliosides (GM), including GM1, has recently been reported in the brains of Alzheimer's disease (AD) patients. Moreover, amyloid-positive synaptosomes obtained from AD brains were found to contain high-density GM1 clusters, suggesting a pathological significance of GM1 increase at presynaptic neuritic terminals in AD. Here, we show that membrane GM1 specifically recruits small soluble oligomers of the 42-residue form of amyloid-␤ peptide (A␤ 42 ), with intracellular flux of Ca 2+ ions in primary rat hippocampal neurons and in human neuroblastoma cells. Specific membrane proteins appear to be involved in the early and transient influx of Ca 2+ ions induced by A␤ 42 oligomers with high solvent-exposed hydrophobicity (A+), but not in the sustained late influx of the same oligomers and in that induced by A␤ 42 oligomers with low solvent-exposed hydrophobicity (A−) in GM1-enriched cells. In addition, A+ oligomers accumulate in proximity of membrane NMDA and AMPA receptors, inducing the early and transient Ca 2+ influx, although FRET shows that the interaction is not direct. These results suggest that age-dependent clustering of GM1 within neuronal membranes could induce neurodegeneration in elderly people as a consequence of an increased ability of the lipid bilayers to recruit membrane-permeabilizing oligomers. We also show that both lipid and protein components of the plasma membrane can contribute to neuronal dysfunction, thus expanding the molecular targets for therapeutic intervention in AD.

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“…We first compared the toxic properties of the purified α-syn species in human dopaminergic neuroblastoma cell lines (M17 and SH-S5Y5 cells). Using the uptake of the vital dye propidium iodide (PI) as a marker for membrane disruption and toxicity, in combination with flow cytometry quantification, we observed that neither α-syn monomers ( Although several studies have shown that different aggregated forms of α-syn exhibit toxicity in various cellular 17,20,23,32 and in vivo models, 12,32 increasing evidence from our group 27,33 and others 34 suggest that amyloid toxicity could be linked to the process of amyloid formation rather than to specific aggregated forms of amyloidogenic proteins. To determine whether this applies to α-syn-induced toxicity, we assessed the effect of inducing fibril growth by the addition of α-syn PFFs (10%) to monomeric α-syn solutions.…”

Section: Resultsmentioning

confidence: 89%

Fibril growth and seeding capacity play key roles in α-synuclein-mediated apoptotic cell death

et al. 2015

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The role of extracellular α-synuclein (α-syn) in the initiation and the spreading of neurodegeneration in Parkinson's disease (PD) has been studied extensively over the past 10 years. However, the nature of the α-syn toxic species and the molecular mechanisms by which they may contribute to neuronal cell loss remain controversial. In this study, we show that fully characterized recombinant monomeric, fibrillar or stabilized forms of oligomeric α-syn do not trigger significant cell death when added individually to neuroblastoma cell lines. However, a mixture of preformed fibrils (PFFs) with monomeric α-syn becomes toxic under conditions that promote their growth and amyloid formation. In hippocampal primary neurons and ex vivo hippocampal slice cultures, α-syn PFFs are capable of inducing a moderate toxicity over time that is greatly exacerbated upon promoting fibril growth by addition of monomeric α-syn. The causal relationship between α-syn aggregation and cellular toxicity was further investigated by assessing the effect of inhibiting fibrillization on α-syn-induced cell death. Remarkably, our data show that blocking fibril growth by treatment with known pharmacological inhibitor of α-syn fibrillization (Tolcapone) or replacing monomeric α-syn by monomeric β-synuclein in α-syn mixture composition prevent α-syn-induced toxicity in both neuroblastoma cell lines and hippocampal primary neurons. We demonstrate that exogenously added α-syn fibrils bind to the plasma membrane and serve as nucleation sites for the formation of α-syn fibrils and promote the accumulation and internalization of these aggregates that in turn activate both the extrinsic and intrinsic apoptotic cell death pathways in our cellular models. Our results support the hypothesis that ongoing aggregation and fibrillization of extracellular α-syn play central roles in α-syn extracellular toxicity, and suggest that inhibiting fibril growth and seeding capacity constitute a viable strategy for protecting against α-syn-induced toxicity and slowing the progression of neurodegeneration in PD and other synucleinopathies. 1 Nevertheless, the relationship between α-syn aggregation and neurodegeneration in PD remains elusive. 2A possible role for extracellular α-syn in the pathogenicity of PD emerged from the observation that newly grafted neurons in PD patients exhibit α-syn pathology similar to that of neighboring diseased cells. 3,4 Despite the consensus that α-syn is mainly an intracellular protein, α-syn has been detected in the cerebrospinal fluid under both pathological and healthy conditions. 5 In addition, in vivo rodent models and cellular studies have shown that monomers 6 and aggregated forms 6,7 of α-syn are secreted into the extracellular space via several mechanisms, 7,8 including the nonclassical endoplasmic reticulum/Golgi-independent exocytosis 8 or the exosomal route, 9,10 and are then internalized by neighboring cells. 7This suggests that extracellular α-syn may play a critical role in the spreading of α-syn pathology throughout the brai...

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Nucleation-Dependent Polymerization Is an Essential Component of Amyloid-Mediated Neuronal Cell Death

Cited by 209 publications

References 46 publications

Preparation and characterization of toxic Aβ aggregates for structural and functional studies in Alzheimer's disease research

Preparation and characterization of toxic Aβ aggregates for structural and functional studies in Alzheimer's disease research

Soluble Oligomers Require a Ganglioside to Trigger Neuronal Calcium Overload

Fibril growth and seeding capacity play key roles in α-synuclein-mediated apoptotic cell death

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