Identification of the Sites of Tau Hyperphosphorylation and Activation of Tau Kinases in Synucleinopathies and Alzheimer’s Diseases

Duka, Valeriy; Lee, Jae Hoon; Credle, Joel J.; Wills, Jonathan; Oaks, Adam W.; Smolinsky, Ciaran; Shah, K.; Mash, Deborah C.; Masliah, Eliezer; Sidhu, Anita

doi:10.1371/journal.pone.0075025

Cited by 91 publications

(84 citation statements)

References 36 publications

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“…As expected, elevated levels of α-Syn immunostaining were also seen in LBs of PD SN neurons ( Figure 2i, lower panel). Although we have analyzed total GSK-3β and p-GSK-3β-S9 in brains of PD patients by immunoblotting, 12,13 this is the first study to provide direct immunopositive evidence of increased p-GSK-3β-Y216 expression in DA-neurons of SN from PD patients.…”

Section: Resultsmentioning

confidence: 98%

“…In postmortem PD striatum, we have recently examined 20 different epitopes of p-Tau and found hyperphosphorylation to occur at 10 sites. 12 We, therefore, examined the pattern of Tau hyperphosphorylation by immunoblotting at these 10 epitopes in midbrain (Figures 3a and b), striatum (Figures 3c and d), and frontal cortex (Figures 3e and f) of 15-month-old TG and control mice. In midbrain, significant hyperphosphorylation was seen at 8 of the 10 epitopes examined (T205, T212, S235, S262, S356, S396/404, S409, and S422).…”

Section: Resultsmentioning

confidence: 99%

“…Tissues were prepared as previously described. 12,19,20 See supplementary material and methods for further details.…”

Section: Diffusion Tensor Mri Mri Was Performed At the Preclinical Imentioning

confidence: 99%

“…Western blot analyses of mouse tissue homogenates were performed as previously described. 12 See supplementary material and methods for further details.…”

Section: Diffusion Tensor Mri Mri Was Performed At the Preclinical Imentioning

confidence: 99%

“…12,13,16,19,20 In in vitro studies of MPTPtreated SH-SY5Y cells, blockade of GSK-3β with lithium, or with the highly selective non-ATP competitive inhibitor, TDZD--8, prevented the induction of p-GSK-3β-Y216, abolished p-Tau formation, and reversed the accumulation and aggregation of both p-Tau and α-Syn, averting cell death. 16 Other studies using Rotenone or MPTP/MPP+ in chemical PD models, have shown similar results of decreased neuronal viability during treatments accompanied by dose-and timedependent increases in GSK-3β activation, with decreased cytotoxicity detected when GSK-3β was inhibited or knockeddown through the use of GSK-3β-specific small molecule inhibitors or through RNAi.…”

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confidence: 99%

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GSK-3β dysregulation contributes to parkinson’s-like pathophysiology with associated region-specific phosphorylation and accumulation of tau and α-synuclein

et al. 2014

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Aberrant posttranslational modifications (PTMs) of proteins, namely phosphorylation, induce abnormalities in the biological properties of recipient proteins, underlying neurological diseases including Parkinson's disease (PD). Genome-wide studies link genes encoding α-synuclein (α-Syn) and Tau as two of the most important in the genesis of PD. Although several kinases are known to phosphorylate α-Syn and Tau, we focused our analysis on GSK-3β because of its accepted role in phosphorylating Tau and to increasing evidence supporting a strong biophysical relationship between α-Syn and Tau in PD. Therefore, we investigated transgenic mice, which express a point mutant (S9A) of human GSK-3β. GSK-3β-S9A is capable of activation through endogenous natural signaling events, yet is unable to become inactivated through phosphorylation at serine-9. We used behavioral, biochemical, and in vitro analysis to assess the contributions of GSK-3β to both α-Syn and Tau phosphorylation. Behavioral studies revealed progressive age-dependent impairment of motor function, accompanied by loss of tyrosine hydroxylase-positive (TH+ DA-neurons) neurons and dopamine production in the oldest age group. Magnetic resonance imaging revealed deterioration of the substantia nigra in aged mice, a characteristic feature of PD patients. At the molecular level, kinase-active p-GSK-3β-Y216 was seen at all ages throughout the brain, yet elevated levels of p-α-Syn-S129 and p-Tau (S396/404) were found to increase with age exclusively in TH+ DA-neurons of the midbrain. p-GSK-3β-Y216 colocalized with p-Tau and p-α-Syn-S129. In vitro kinase assays showed that recombinant human GSK-3β directly phosphorylated α-Syn at a single site, Ser129, in addition to its known ability to phosphorylate Tau. Moreover, α-Syn and Tau together cooperated with one another to increase the magnitude or rate of phosphorylation of the other by GSK-3β. Together, these data establish a novel upstream role for GSK-3β as one of several kinases associated with PTMs of key proteins known to be causal in PD.

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Section: Resultsmentioning

confidence: 98%

Section: Resultsmentioning

confidence: 99%

“…Tissues were prepared as previously described. 12,19,20 See supplementary material and methods for further details.…”

Section: Diffusion Tensor Mri Mri Was Performed At the Preclinical Imentioning

confidence: 99%

“…Western blot analyses of mouse tissue homogenates were performed as previously described. 12 See supplementary material and methods for further details.…”

Section: Diffusion Tensor Mri Mri Was Performed At the Preclinical Imentioning

confidence: 99%

mentioning

confidence: 99%

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GSK-3β dysregulation contributes to parkinson’s-like pathophysiology with associated region-specific phosphorylation and accumulation of tau and α-synuclein

et al. 2014

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Plasma P‐tau181 to Aβ42 ratio is associated with brain amyloid burden and hippocampal atrophy in an Asian cohort of Alzheimer's disease patients with concomitant cerebrovascular disease

Chong

Ashton

Karikari

et al. 2021

Alzheimer's & Dementia

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Introduction:There is increasing evidence that phosphorylated tau (P-tau181) is a specific biomarker for Alzheimer's disease (AD) pathology, but its potential utility in non-White patient cohorts and patients with concomitant cerebrovascular disease (CeVD) is unknown. Methods: Single molecule array (Simoa) measurements of plasma P-tau181, total tau, amyloid beta (Aβ)40 and Aβ42, as well as derived ratios were correlated with neuroimaging modalities indicating brain amyloid (Aβ+), hippocampal atrophy, and CeVD in a Singapore-based cohort of non-cognitively impaired (NCI; n = 43), cognitively impaired no dementia (CIND; n = 91), AD (n = 44), and vascular dementia (VaD; n = 22) subjects.

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Sleep Deprivation Affects Tau Phosphorylation in Human Cerebrospinal Fluid

Barthélemy

Liu

et al. 2020

Annals of Neurology

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Tau hyperphosphorylation is an early step in tau-mediated neurodegeneration and is associated with intracellular aggregation of tau as neurofibrillary tangles, neuronal and synaptic loss, and eventual cognitive dysfunction in Alzheimer disease. Sleep loss increases the cerebrospinal fluid concentration of amyloid-β and tau. Using mass spectrometry, we measured tau and phosphorylated tau concentrations in serial samples of cerebrospinal fluid collected from participants who were sleep-deprived, treated with sodium oxybate, or allowed to sleep normally. We found that sleep loss affected phosphorylated tau differently depending on the modified site. These findings suggest a mechanism for sleep loss to increase risk of Alzheimer disease.

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Identification of the Sites of Tau Hyperphosphorylation and Activation of Tau Kinases in Synucleinopathies and Alzheimer’s Diseases

Cited by 91 publications

References 36 publications

GSK-3β dysregulation contributes to parkinson’s-like pathophysiology with associated region-specific phosphorylation and accumulation of tau and α-synuclein

GSK-3β dysregulation contributes to parkinson’s-like pathophysiology with associated region-specific phosphorylation and accumulation of tau and α-synuclein

Plasma P‐tau181 to Aβ42 ratio is associated with brain amyloid burden and hippocampal atrophy in an Asian cohort of Alzheimer's disease patients with concomitant cerebrovascular disease

Sleep Deprivation Affects Tau Phosphorylation in Human Cerebrospinal Fluid

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