The active Hsc70/tau complex can be exploited to enhance tau turnover without damaging microtubule dynamics

Fontaine, Sarah N.; Martin, Mackenzie D.; Akoury, Elias; Assimon, Victoria A.; Borysov, Sergiy; Nordhues, Bryce A.; Sabbagh, Jonathan J.; Cockman, Matt; Gestwicki, Jason E.; Zweckstetter, Markus; Dickey, Chad A.

doi:10.1093/hmg/ddv135

Cited by 28 publications

(41 citation statements)

References 56 publications

(73 reference statements)

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“…NMR studies of Hsc70 binding to tau2N4R show that Hsc70 causes slight broadening in peaks corresponding to residues 375-380 of tau2N4R, though this broadening is not as strong as that of the 275 VQIINK 280 and 306 VQIVYK 311 motifs (22,23). Because we found similar Hsc70 chaperone activity against tau4RD, which does not contain these residues, and tau2N4R, which does, we believe that this interaction does not significantly alter Hsc70's mechanism of action.…”

Section: Discussionmentioning

confidence: 58%

“…Individuals carrying diseaseassociated mutations in the tau gene that enhance aggregation propensity only develop symptoms later in life (19), suggesting that neuronal cells have the machinery to maintain aggregation-prone tau in a soluble form for years. Interactions between tau and a number of chaperones have been documented, indicating that multiple players within the chaperone network are involved in this process (20)(21)(22)(23)(24)(25). However, the mechanisms by which these chaperones interact with tau and their effects on tau fibril formation remain unclear.…”

mentioning

confidence: 99%

“…However, ATP-independent activity has also been reported in Hsp70-family chaperones (33)(34)(35). Hsc70 binds to the two aggregation-prone motifs in tau and has been proposed as a pharmacological target (22,23,36). Its overexpression leads to an increase in the concentration of tau in cell culture models, while an Hsc70 inhibitor causes a decrease in tau concentration in cell cultures and rescues long-term potentiation deficits in tauopathy model mouse brain slices (22,36).…”

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confidence: 99%

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HspB1 and Hsc70 chaperones engage distinct tau species and have different inhibitory effects on amyloid formation

Baughman

Clouser

Klevit

et al. 2018

Journal of Biological Chemistry

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The microtubule-associated protein tau forms insoluble, amyloid-type aggregates in various dementias, most notably Alzheimer's disease. Cellular chaperone proteins play important roles in maintaining protein solubility and preventing aggregation in the crowded cellular environment. While tau is known to interact with numerous chaperones, it remains unclear how these chaperones function mechanistically to prevent tau aggregation and how chaperones from different classes compare in terms of mechanism. Here, we focused on the small heat shock protein HspB1 and the constitutive chaperone Hsc70 (also known as HspA8), and report how each chaperone interacts with tau to prevent its fibril formation. Using fluorescence and NMR spectroscopy, we show that the two chaperones inhibit tau fibril formation by distinct mechanisms. HspB1 delayed tau fibril formation by weakly interacting with early species in the aggregation process, while Hsc70 was highly efficient at preventing tau fibril elongation possibly by capping the ends of tau fibrils. Both chaperones recognized aggregation-prone motifs within the microtubule-binding repeat region of tau. However, HspB1 binding remained transient in both aggregation-promoting and nonaggregating conditions, whereas Hsc70 binding was significantly tighter under aggregationpromoting conditions. These differences highlight the fact that chaperones from different families play distinct but complementary roles in the prevention of pathological protein aggregation.

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Section: Discussionmentioning

confidence: 58%

mentioning

confidence: 99%

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confidence: 99%

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HspB1 and Hsc70 chaperones engage distinct tau species and have different inhibitory effects on amyloid formation

Baughman

Clouser

Klevit

et al. 2018

Journal of Biological Chemistry

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“…CHIP-mediated ubiquitination of phosphorylated tau results in decreased cell death [140, 141] and deletion of CHIP results in the accumulation of hyperphosphorylated tau [142, 143]. Interestingly, the Hsp70 family member, Hsc70, interacts with tau with greater affinity than Hsp72 and stabilizes tau [137, 144], and expression of a dominant-negative variant of Hsc70 led to clearance of tau via the proteasome in HEK293T cells, as well as in brain tissue [145]. …”

Section: Improving Cellular Proteostasismentioning

confidence: 99%

Therapeutic strategies for the treatment of tauopathies: Hopes and challenges

Khanna

Kovalevich

Lee

et al. 2016

Alzheimer's & Dementia

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A group of neurodegenerative diseases referred to as tauopathies are characterized by the presence of brain cells harboring inclusions of pathological species of the tau protein. These disorders include Alzheimer’s disease (AD) and frontotemporal lobar degeneration (FTLD) due to tau pathology, including progressive supranuclear palsy, corticobasal degeneration and Pick’s disease. Tau is normally a microtubule-associated protein that appears to play an important role in ensuring proper axonal transport, but in tauopathies tau becomes hyperphosphorylated and disengages from microtubules, with consequent misfolding and deposition into inclusions that mainly affect neurons, but also glia. A body of experimental evidence suggests that the development of tau inclusions leads to the neurodegeneration observed in tauopathies, and there is a growing interest in developing tau-directed therapeutic agents. The following review provides a summary of strategies under investigation for the potential treatment of tauopathies, highlighting both the promises and challenges associated with these various therapeutic approaches.

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“…12 In particular, inhibitors of the heat shock protein 70 kDa (Hsp70) chaperone family are highly effective at lowering tau. 8,14 When the activity of these molecular chaperones is pharmacologically or even genetically inhibited, tau can be degraded. 15–18 Recently, a number of other small molecules with anti-Hsp70 activity have been described.…”

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confidence: 99%

Inhibition of Both Hsp70 Activity and Tau Aggregation in Vitro Best Predicts Tau Lowering Activity of Small Molecules

et al. 2016

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Three scaffolds with inhibitory activity against the heat shock protein 70 (Hsp70) family of chaperones have been found to enhance the degradation of the microtubule associated protein tau in cells, neurons, and brain tissue. This is important because tau accumulation is linked to neurodegenerative diseases including Alzheimer’s disease (AD) and chronic traumatic encephalopathy (CTE). Here, we expanded upon this study to investigate the anti-tau efficacy of additional scaffolds with Hsp70 inhibitory activity. Five of the nine scaffolds tested lowered tau levels, with the rhodacyanine and phenothiazine scaffolds exhibiting the highest potency as previously described. Because phenothiazines also inhibit tau aggregation in vitro, we suspected that this activity might be a more accurate predictor of tau lowering. Interestingly, the rhodacyanines did inhibit in vitro tau aggregation to a similar degree as phenothiazines, correlating well with tau-lowering efficacy in cells and ex vivo slices. Moreover, other Hsp70 inhibitor scaffolds with weaker tau-lowering activity in cells inhibited tau aggregation in vitro, albeit at lower potencies. When we tested six well-characterized tau aggregation inhibitors, we determined that this mechanism of action was not a better predictor of tau-lowering than Hsp70 inhibition. Instead, we found that compounds possessing both activities were the most effective at promoting tau clearance. Moreover, cytotoxicity and PAINS activity are critical factors that can lead to false-positive lead identification. Strategies designed around these principles will likely yield more efficacious tau-lowering compounds.

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The active Hsc70/tau complex can be exploited to enhance tau turnover without damaging microtubule dynamics

Cited by 28 publications

References 56 publications

HspB1 and Hsc70 chaperones engage distinct tau species and have different inhibitory effects on amyloid formation

HspB1 and Hsc70 chaperones engage distinct tau species and have different inhibitory effects on amyloid formation

Therapeutic strategies for the treatment of tauopathies: Hopes and challenges

Inhibition of Both Hsp70 Activity and Tau Aggregation in Vitro Best Predicts Tau Lowering Activity of Small Molecules

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