Activation of Hsp70 reduces neurotoxicity by promoting polyglutamine protein degradation

Wang, Adrienne M.; Miyata, Yoshinari; Klinedinst, Susan; Peng, Hwei Ming; Chua, Jason P.; Komiyama, Tomoko; Li, Xiaokai; Morishima, Yosuke; Merry, Diane E.; Pratt, William B.; Osawa, Yoichi; Collins, Catherine A.; Gestwicki, Jason E.; Lieberman, Andrew P.

doi:10.1038/nchembio.1140

Cited by 160 publications

(209 citation statements)

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“…Hsp70 has been shown to inhibit aggregation and toxicity of a variety of amyloidogenic systems via distinct mechanisms (28)(29)(30). Here we show that hsp70 is able to protect cells against the deleterious effects of β 2 m fibril-mediated cell dysfunction to a greater extent than chemical cross-linking.…”

Section: Discussionmentioning

confidence: 60%

“…To determine whether fibrilinduced membrane damage can be inhibited by enhancing the kinetic stability of β 2 m amyloid fibrils, the molecular chaperone hsp70 was added. Previous studies have shown that the association of hsp70 (or its constitutively expressed homolog, hsc70) with amyloid aggregates protects against amyloid toxicity (28)(29)(30). Recombinant hsp70-1A (29) was incubated with β 2 m amyloid fibrils at pH 6.4 in a 1:0.25 or 1:3 molar ratio (monomer equivalent β 2 m:chaperone) and the effect of the chaperone on fibril stability was measured using ThT fluorescence.…”

Section: Restricting Molecular Shedding Decreases Membrane Damage Andmentioning

confidence: 99%

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pH-induced molecular shedding drives the formation of amyloid fibril-derived oligomers

Tipping

Karamanos

Jakhria

et al. 2015

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

104

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Amyloid disorders cause debilitating illnesses through the formation of toxic protein aggregates. The mechanisms of amyloid toxicity and the nature of species responsible for mediating cellular dysfunction remain unclear. Here, using β 2 -microglobulin (β 2 m) as a model system, we show that the disruption of membranes by amyloid fibrils is caused by the molecular shedding of membrane-active oligomers in a process that is dependent on pH. Using thioflavin T (ThT) fluorescence, NMR, EM and fluorescence correlation spectroscopy (FCS), we show that fibril disassembly at pH 6.4 results in the formation of nonnative spherical oligomers that disrupt synthetic membranes. By contrast, fibril dissociation at pH 7.4 results in the formation of nontoxic, native monomers. Chemical cross-linking or interaction with hsp70 increases the kinetic stability of fibrils and decreases their capacity to cause membrane disruption and cellular dysfunction. The results demonstrate how pH can modulate the deleterious effects of preformed amyloid aggregates and suggest why endocytic trafficking through acidic compartments may be a key factor in amyloid disease.amyloid | fibrils | disassembly | oligomer | membrane disruption

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Section: Discussionmentioning

confidence: 60%

Section: Restricting Molecular Shedding Decreases Membrane Damage Andmentioning

confidence: 99%

pH-induced molecular shedding drives the formation of amyloid fibril-derived oligomers

Tipping

Karamanos

Jakhria

et al. 2015

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

104

View full text Add to dashboard Cite

show abstract

“…Studies with the small molecule geldanamycin (GA), a potent inhibitor of Hsp90 ATPase activity, have revealed that increases in the levels of molecular chaperones such as Hsp70 or Hsp40 are associated with reduced aggregation and toxicity of mutant HTTex1 fragments in cells and flies [36]. The importance of chaperone networks in managing misfolded proteins in cells is also supported by the effect of the compound YM-1, which increases the binding affinity of Hsp70 to polyQ disease proteins, leading to an increased efficiency of their ubiquitination and degradation [37]. High-throughput screenings have led to the identification of numerous novel small molecules that influence the expression of molecular chaperones in mammalian cells [38].…”

Section: Identification Of Small Molecules That Influence Polyq-mediamentioning

confidence: 99%

Spontaneous self-assembly of pathogenic huntingtin exon 1 protein into amyloid structures

Trepte

Strempel

Wanker

2014

Essays in Biochemistry

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Published in final edited form as:Trepte, P., Strempel, N., Wanker, E.E. Spontaneous self-assembly of pathogenic huntingtin exon 1 protein into amyloid structures. Abstract:Polyglutamine ( This chapter reviews the current literature regarding misfolding and aggregation of polyQ-containing disease proteins. We specifically focus on studies that have investigated the amyloidogenesis of polyQ-containing huntingtin exon 1 (HTTex1) fragments. These protein fragments are disease-relevant and play a critical role in HD pathogenesis. We will outline potential mechanisms behind mutant HTTex1 aggregation and toxicity, as well as proteins and small molecules that can modify HTTex1 amyloidogenesis in vitro and in vivo. The potential implications of such studies for the development of novel therapeutic strategies are discussed.

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“…However, trails using antiandrogen therapy, commonly used in the treatment of advanced prostate cancer, yielded disappointing findings, despite highly promising animal studies. Other studies have shown AR:HSP70 complex and small molecules such as trehalose as a potential therapeutic target for SBMA [25,28]. Based on these studies, a potential therapeutic model can be proposed (Figure 2).…”

mentioning

confidence: 99%

Spinal bulbar muscular atrophy, an inherited neurodegenerative disease: Potential mechanisms and therapeutic targets

Kumar¹

2017

J Syst Integr Neurosci

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Instability of CAG triplet repeat encoding poly-glutamine (polyQ) stretch in the androgen receptor (AR) gene has been implicated as a putative mechanism in spinal bulbar muscular atrophy (SBMA) or Kennedy's disease. Although the underlying mechanisms are not completely understood, suggested pathological pathways of SBMA involve the formation of AR nuclear and cytoplasmic aggregates. Here we discuss the role of polyQ chain length extension in the pathophysiology of SBMA and the potential therapeutic targets.

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Activation of Hsp70 reduces neurotoxicity by promoting polyglutamine protein degradation

Cited by 160 publications

References 50 publications

pH-induced molecular shedding drives the formation of amyloid fibril-derived oligomers

pH-induced molecular shedding drives the formation of amyloid fibril-derived oligomers

Spontaneous self-assembly of pathogenic huntingtin exon 1 protein into amyloid structures

Spinal bulbar muscular atrophy, an inherited neurodegenerative disease: Potential mechanisms and therapeutic targets

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