Coyne_2017_Cell.Rep_21_110

Reference

Title : Post-transcriptional Inhibition of Hsc70-4\/HSPA8 Expression Leads to Synaptic Vesicle Cycling Defects in Multiple Models of ALS - Coyne_2017_Cell.Rep_21_110
Author(s) : Coyne AN , Lorenzini I , Chou CC , Torvund M , Rogers RS , Starr A , Zaepfel BL , Levy J , Johannesmeyer J , Schwartz JC , Nishimune H , Zinsmaier K , Rossoll W , Sattler R , Zarnescu DC
Ref : Cell Rep , 21 :110 , 2017
Abstract :

Amyotrophic lateral sclerosis (ALS) is a synaptopathy accompanied by the presence of cytoplasmic aggregates containing TDP-43, an RNA-binding protein linked to approximately 97% of ALS cases. Using a Drosophila model of ALS, we show that TDP-43 overexpression (OE) in motor neurons results in decreased expression of the Hsc70-4 chaperone at the neuromuscular junction (NMJ). Mechanistically, mutant TDP-43 sequesters hsc70-4 mRNA and impairs its translation. Expression of the Hsc70-4 ortholog, HSPA8, is also reduced in primary motor neurons and NMJs of mice expressing mutant TDP-43. Electrophysiology, imaging, and genetic interaction experiments reveal TDP-43-dependent defects in synaptic vesicle endocytosis. These deficits can be partially restored by OE of Hsc70-4, cysteine-string protein (Csp), or dynamin. This suggests that TDP-43 toxicity results in part from impaired activity of the synaptic CSP/Hsc70 chaperone complex impacting dynamin function. Finally, Hsc70-4/HSPA8 expression is also post-transcriptionally reduced in fly and human induced pluripotent stem cell (iPSC) C9orf72 models, suggesting a common disease pathomechanism.

PubMedSearch : Coyne_2017_Cell.Rep_21_110
PubMedID: 28978466

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Citations formats

Coyne AN, Lorenzini I, Chou CC, Torvund M, Rogers RS, Starr A, Zaepfel BL, Levy J, Johannesmeyer J, Schwartz JC, Nishimune H, Zinsmaier K, Rossoll W, Sattler R, Zarnescu DC (2017)
Post-transcriptional Inhibition of Hsc70-4\/HSPA8 Expression Leads to Synaptic Vesicle Cycling Defects in Multiple Models of ALS
Cell Rep 21 :110

Coyne AN, Lorenzini I, Chou CC, Torvund M, Rogers RS, Starr A, Zaepfel BL, Levy J, Johannesmeyer J, Schwartz JC, Nishimune H, Zinsmaier K, Rossoll W, Sattler R, Zarnescu DC (2017)
Cell Rep 21 :110