α-Synuclein Targets the Plasma Membrane via the Secretory Pathway and Induces Toxicity in Yeast

Dixon, Cheryl; Mathias, Neal; Zweig, Richard M.; Davis, Donnie A.; Gross, David S.

doi:10.1534/genetics.104.035493

Cited by 107 publications

(114 citation statements)

References 63 publications

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“…In conclusion, we support a model of yeast toxicity in which overexpressed monomeric synuclein directly coats the plasma and internal membranes via its amphipathic α-helices, disrupting normal membrane processes (including vesicle trafficking [19][20][21], and eventually leading to toxicity. Perhaps the simplest mechanism by which synuclein binding could disrupt membrane processes is a non-specific one.…”

Section: Is Membrane Binding Necessary For Synuclein Induced Yeast Tosupporting

confidence: 73%

“…18,19 Wild type and A53T α-synuclein are both toxic and localize to inclusions and the plasma membrane when expressed from multiple GAL promoters, such as those on 2-micron plasmids (high copy number) or from multiple integrated copies. 18,20,21 In contrast, the A30P variant is non-toxic to yeast and is uniformly distributed throughout the cytoplasm. 18 All of the synuclein proteins are relatively non-toxic when expressed from a single copy.…”

Section: Introductionmentioning

confidence: 99%

“…1; discussed below). Dixon et al 21 showed that mutation of proteins in the yeast secretory pathway (including ER-Golgi transport) can cause α-synuclein to change its localization from plasma membrane to punctate inclusions. It was later shown that α-synuclein itself can disrupt ER-Golgi trafficking.…”

mentioning

confidence: 99%

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Relationships between the Sequence of α-Synuclein and its Membrane Affinity, Fibrillization Propensity, and Yeast Toxicity

Volles

Lansbury

2007

Journal of Molecular Biology

223

206

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SummaryTo investigate the α-synuclein protein and its role in Parkinson's disease, we screened a library of random point mutants both in vitro and in yeast to find variants in an unbiased way that could help us understand the sequence-phenotype relationship. We developed a rapid purification method that allowed us to screen 59 synuclein mutants in vitro and discovered two double point mutants that fibrillized slowly relative to wild type, A30P, and A53T α-synucleins. The yeast toxicity of all of these proteins was measured and we found no correlation with fibrillization rate, suggesting that fibrillization is not necessary for synuclein-induced yeast toxicity. We also found that β-synuclein was of intermediate toxicity to yeast and γ-synuclein was non-toxic. Coexpression of Parkinson's disease related genes DJ-1, parkin, Pink1, UCH-L1, or synphilin, with synuclein, did not affect synuclein toxicity. A second screen, of several thousand library clones in yeast, identified 25 nontoxic α-synuclein sequence variants. Most of these contained a mutation to either proline or glutamic acid that caused a defect in membrane binding. We hypothesize that yeast toxicity is caused by synuclein binding directly to membranes at levels sufficient to non-specifically disrupt homeostasis.

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Section: Is Membrane Binding Necessary For Synuclein Induced Yeast Tosupporting

confidence: 73%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Relationships between the Sequence of α-Synuclein and its Membrane Affinity, Fibrillization Propensity, and Yeast Toxicity

Volles

Lansbury

2007

Journal of Molecular Biology

223

206

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“…In immunogold electron microscopy examination of rat brain neurons, the αSyn concentration was found to be higher in endoplasmic reticulum (ER) than in cytoplasmic region (Zhang et al 2008). Synthesized αSyn in yeast was found to be translocated from the ER to the Golgi and further to the plasma membrane through a classical secretion pathway (Dixon et al 2005). Recently, αSyn has been reported to be involved in the impairment of ER functions.…”

Section: Introductionmentioning

confidence: 99%

Domain a’ of protein disulfide isomerase plays key role in inhibiting α-synuclein fibril formation

Cheng

Wang

2010

Cell Stress and Chaperones

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α-Synuclein (αSyn) is the main component of Lewy bodies formed in midbrain dopaminergic neurons which is a pathological characteristic of Parkinson's disease. It has been recently showed to induce endoplasmic reticulum (ER) stress and impair ER functions. However, the mechanism of how ER responds to αSyn toxicity is poorly understood. In the present study, we found that protein disulfide isomerase (PDI), a stress protein abundant in ER, effectively inhibits αSyn fibril formation in vitro. In PDI molecule with a structure of abb'xa'c, domain a' was found to be essential and sufficient for PDI to inhibit αSyn fibril formation. PDI was further found to be more avid for binding with intermediate species formed during αSyn fibril formation, and the binding was more intensive in the later lag phase. Our results provide new insight into the role of PDI in protecting ER from the deleterious effects of misfolded protein accumulation in many neurodegenerative diseases.

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“…Much of what now is known about these processes was discovered first in yeast and later applied to cells of higher organisms, including neurons. In yeast, however, secretion is constitutive, allowing vesicles to fuse with the plasma membrane without an external signal (15). In neurons, in contrast, presynaptic vesicles fuse with the plasma membrane in a controlled manner.…”

mentioning

confidence: 99%

Splice isoform and pharmacological studies reveal that sterol depletion relocalizes α-synuclein and enhances its toxicity

Valastyan¹,

Termine²,

Lindquist³

2014

Proc. Natl. Acad. Sci. U.S.A.

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Synucleinopathies are neurodegenerative diseases associated with toxicity of the lipid-binding protein α-synuclein (α-syn). When expressed in yeast, α-syn associates with membranes at the endoplasmic reticulum and traffics with vesicles out to the plasma membrane. At higher levels it elicits a number of phenotypes, including blocking vesicle trafficking. The expression of α-syn splice isoforms varies with disease, but how these isoforms affect protein function is unknown. We investigated two of the most abundant isoforms, resulting in deletion of exon four (α-synΔ4) or exon six (α-synΔ6). α-SynΔ4, missing part of the lipid-binding domain, had reduced toxicity and membrane binding. α-SynΔ6, missing part of the protein-protein interaction domain, had reduced toxicity but no reduction in membrane binding. To compare the mechanism by which the splice isoforms exert toxicity, equally toxic strains were probed with genetic modifiers of α-syn-induced toxicity. Most modifiers equally altered the toxicity induced by the splice isoforms and full-length α-syn (α-synFL). However, the splice isoform strains responded differently to a sterol-binding protein, leading us to examine the effect of sterols on α-syn-induced toxicity. Upon inhibition of sterol synthesis, α-synFL and α-synΔ6, but not α-synΔ4, showed decreased plasma membrane association, increased vesicular association, and increased cellular toxicity. Thus, higher membrane sterol concentrations favor plasma membrane binding of α-synFL and α-synΔ6 and may be protective of synucleinopathy progression. Given the common use of cholesterol-reducing statins and these potential effects on membrane binding proteins, further investigation of how sterol concentration and α-syn splice isoforms affect vesicular trafficking in synucleinopathies is warranted.

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α-Synuclein Targets the Plasma Membrane via the Secretory Pathway and Induces Toxicity in Yeast

Cited by 107 publications

References 63 publications

Relationships between the Sequence of α-Synuclein and its Membrane Affinity, Fibrillization Propensity, and Yeast Toxicity

Relationships between the Sequence of α-Synuclein and its Membrane Affinity, Fibrillization Propensity, and Yeast Toxicity

Domain a’ of protein disulfide isomerase plays key role in inhibiting α-synuclein fibril formation

Splice isoform and pharmacological studies reveal that sterol depletion relocalizes α-synuclein and enhances its toxicity

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