Effects of oligomer toxicity, fibril toxicity and fibril spreading in synucleinopathies

Cascella, Roberta; Bigi, Alessandra; Cremades, Nunilo; Cecchi, Cristina

doi:10.1007/s00018-022-04166-9

Cited by 59 publications

(51 citation statements)

References 232 publications

(370 reference statements)

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“…A potential and so far speculative explanation could be that Lamp1 protects against α-synuclein in flies by promoting the formation of innocuous aggregates of this protein, which would tend to accumulate as they are not easily degraded and which could also be more easily detected by immunostaining than the soluble forms. In the absence of Lamp1, a larger part of α-synA30P would remain monomeric in the cytoplasm or, more likely, owing to its aggregation properties, form soluble oligomers, which are known to be the more toxic species of this protein [ 27 ].…”

Section: Discussionmentioning

confidence: 99%

Lamp1 Deficiency Enhances Sensitivity to α-Synuclein and Oxidative Stress in Drosophila Models of Parkinson Disease

Rahmani

Surabhi

Rojo-Cortés

et al. 2022

IJMS

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Parkinson disease (PD) is a common neurodegenerative condition affecting people predominantly at old age that is characterized by a progressive loss of midbrain dopaminergic neurons and by the accumulation of α-synuclein-containing intraneuronal inclusions known as Lewy bodies. Defects in cellular degradation processes such as the autophagy-lysosomal pathway are suspected to be involved in PD progression. The mammalian Lysosomal-associated membrane proteins LAMP1 and LAMP2 are transmembrane glycoproteins localized in lysosomes and late endosomes that are involved in autophagosome/lysosome maturation and function. Here, we show that the lack of Drosophila Lamp1, the homolog of LAMP1 and LAMP2, severely increased fly susceptibility to paraquat, a pro-oxidant compound known as a potential PD inducer in humans. Moreover, the loss of Lamp1 also exacerbated the progressive locomotor defects induced by the expression of PD-associated mutant α-synuclein A30P (α-synA30P) in dopaminergic neurons. Remarkably, the ubiquitous re-expression of Lamp1 in a mutant context fully suppressed all these defects and conferred significant resistance towards both PD factors above that of wild-type flies. Immunostaining analysis showed that the brain levels of α-synA30P were unexpectedly decreased in young adult Lamp1-deficient flies expressing this protein in comparison to non-mutant controls. This suggests that Lamp1 could neutralize α-synuclein toxicity by promoting the formation of non-pathogenic aggregates in neurons. Overall, our findings reveal a novel role for Drosophila Lamp1 in protecting against oxidative stress and α-synuclein neurotoxicity in PD models, thus furthering our understanding of the function of its mammalian homologs.

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Section: Discussionmentioning

confidence: 99%

Lamp1 Deficiency Enhances Sensitivity to α-Synuclein and Oxidative Stress in Drosophila Models of Parkinson Disease

Rahmani

Surabhi

Rojo-Cortés

et al. 2022

IJMS

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“…As illustrated by Cascella et al (2022) the detection of oligomers in situ is complicated by the lack of methods to detect these species specifically in vivo and in patient tissues, although interesting results have been obtained with α-syn proximity ligation assay ( Roberts et al, 2015 ). Using mouse anti-α-syn antibody appropriately conjugated with activated oligonucleotides by Duolink ® kits, in medulla, midbrain and cingulate cortex from PD subjects, abundant amounts of oligomers were demonstrated ( Roberts et al, 2015 ).…”

Section: Oligomers and Neurotoxicitymentioning

confidence: 99%

“…Alpha-syn fibril polymorphism has been ascertained by cryo-electron microscopy but a clear understanding of the structure of α-synOs is still lacking ( Li et al, 2018 ; Du et al, 2022 ). The antiparallel intermolecular β-sheet structure has been observed in a stable, particularly toxic oligomeric form of α-syn and has been proposed as distinctive of α-synOs toxic species ( Celej et al, 2012 ; Cascella et al, 2022 ).…”

Section: Oligomers and Neurotoxicitymentioning

confidence: 99%

Oligomeropathies, inflammation and prion protein binding

2022

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The central role of oligomers, small soluble aggregates of misfolded proteins, in the pathogenesis of neurodegenerative disorders is recognized in numerous experimental conditions and is compatible with clinical evidence. To underline this concept, some years ago we coined the term oligomeropathies to define the common mechanism of action of protein misfolding diseases like Alzheimer, Parkinson or prion diseases. Using simple experimental conditions, with direct application of synthetic β amyloid or α-synuclein oligomers intraventricularly at micromolar concentrations, we could detect differences and similarities in the biological consequences. The two oligomer species affected cognitive behavior, neuronal dysfunction and cerebral inflammatory reactions with distinct mechanisms. In these experimental conditions the proposed mediatory role of cellular prion protein in oligomer activities was not confirmed. Together with oligomers, inflammation at different levels can be important early in neurodegenerative disorders; both β amyloid and α-synuclein oligomers induce inflammation and its control strongly affects neuronal dysfunction. This review summarizes our studies with β-amyloid or α-synuclein oligomers, also considering the potential curative role of doxycycline, a well-known antibiotic with anti-amyloidogenic and anti-inflammatory activities. These actions are analyzed in terms of the therapeutic prospects.

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“…Additional open questions are also concerned with LBs’ pathology: nigrostriatal cell death occurs very early when LBs are not detectable [ 6 ]; LBs do not correlate with symptom severity, and LBs can be incidentally found in the brains of healthy elderly individuals [ 255 , 256 ] or be even absent in some genetic forms of PD [ 257 , 258 ]. Moreover, recent evidence suggests that α-Syn oligomeric species are more toxic than its more aggregated forms [ 259 , 260 , 261 ]. In accordance, α-Syn oligomers differ from LBs in their topographical distribution—the former being more diffuse in the neocortex and the latter more abundant in the brainstem—they are not found in control subjects and correlate with severity of cognitive impairment [ 262 ].…”

Section: Challenges Of Genetic-driven Disease-modifying Therapiesmentioning

confidence: 99%

Precision Medicine in Parkinson’s Disease: From Genetic Risk Signals to Personalized Therapy

et al. 2022

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Understanding the pathophysiology and genetic background of Parkinson’s disease (PD) increases the likelihood of developing effective disease-modifying therapeutic strategies. In particular, the discovery of genetic variants causing or increasing the risk for PD has contributed to refining the clinical, biological, and molecular classification of the disease and has offered new insights into sporadic forms. It is even more evident that specific genetic mutations can show different responses to pharmacological and device-aided therapies. To date, several agents acting on multiple PD-causing pathogenic pathways have been tested as disease-modifying strategies, with disappointing results. This may be caused by the recruitment of PD populations whose underlying molecular pathophysiology is heterogeneous. We believe that an effective model of personalized medicine must be prioritized in the near future. Here, we review the current therapeutic options under clinical and preclinical development for PD and discuss the key pending questions and challenges to face for successful clinical trials. Furthermore, we provide some insights into the role of genetics in guiding the decision-making process on symptomatic and device-aided therapies for PD in daily clinical practice.

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Effects of oligomer toxicity, fibril toxicity and fibril spreading in synucleinopathies

Cited by 59 publications

References 232 publications

Lamp1 Deficiency Enhances Sensitivity to α-Synuclein and Oxidative Stress in Drosophila Models of Parkinson Disease

Lamp1 Deficiency Enhances Sensitivity to α-Synuclein and Oxidative Stress in Drosophila Models of Parkinson Disease

Oligomeropathies, inflammation and prion protein binding

Precision Medicine in Parkinson’s Disease: From Genetic Risk Signals to Personalized Therapy

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