A novel glycogen synthase kinase‐3 inhibitor 2‐methyl‐5‐(3‐{4‐[(<i>S </i>)‐methylsulfinyl]phenyl}‐1‐benzofuran‐5‐yl)‐1,3,4‐oxadiazole decreases tau phosphorylation and ameliorates cognitive deficits in a transgenic model of Alzheimer’s disease

Onishi, Tomohiro; Iwashita, Hiroki; Uno, Yumiko; Kunitomo, Jun-ichi; Saitoh, Morihisa; Kimura, Eiji; Fujita, Hisashi; Uchiyama, Noriko; Kori, Masakuni; Takizawa, Masayuki

doi:10.1111/j.1471-4159.2011.07532.x

Cited by 79 publications

(59 citation statements)

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“…Indeed, an orally administrable-related oxidiazole, 2-methyl-5-(3-{4-[(S)-methylsulfinyl]phenyl}-1-benzofuran-5-yl)-1,3,4-oxadiazole (MMBO), was recently shown to decrease hippocampal Tau phosphorylation at GSK-3 sites, but without affecting Ab pathology, in the 3xTg transgenic AD mouse model. In behavioral assessments, MMBO significantly improved memory deficits in the Y-maze and novel object recognition tests (Onishi et al, 2011). Therefore, these molecules appeared effective in preclinical tests.…”

Section: A Gsk-3b Inhibitor Alleviates Ab 25-35 -Induced Toxicity Andmentioning

confidence: 91%

Blockade of Tau Hyperphosphorylation and Aβ1–42 Generation by the Aminotetrahydrofuran Derivative ANAVEX2-73, a Mixed Muscarinic and σ1 Receptor Agonist, in a Nontransgenic Mouse Model of Alzheimer’s Disease

Lahmy

Meunier²,

Malmström³

et al. 2013

Neuropsychopharmacol

134

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The main objective of the present study was to establish whether the mixed s 1 /muscarinic ligand ANAVEX2-73, shown to be neuroprotective in Alzheimer's disease (AD) models in vivo and currently in clinical phase I/IIa, could have the ability to reduce the appearance of hyperphosphorylated Tau and amyloid-b 1-42 (Ab 1-42 ) in the Ab 25-35 mouse model of AD. We therefore first confirmed that Ab 25-35 injection induced hyperphosphorylation of Tau protein, by showing that it rapidly decreased Akt activity and activated glycogen synthase kinase-3b (GSK-3b) in the mouse hippocampus. Second, we showed that the kinase activation, and resulting Tau alteration, directly contributed to the amyloid toxicity, as co-administration of the selective GSK-3b inhibitor 2-thio(3-iodobenzyl)-5-(1-pyridyl)-[1,3,4]-oxidiazole blocked both Tau phosphorylation and Ab 25-35 -induced memory impairments. Third, we analyzed the ANAVEX2-73 effect on Tau phosphorylation and activation of the related kinase pathways (Akt and GSK-3b). And fourth, we also addressed the impact of the drug on Ab 25-35 -induced Ab 1-42 seeding and observed that the compound significantly blocked the increase in Ab 1-42 and C99 levels in the hippocampus, suggesting that it may alleviate amyloid load in AD models. The comparison with PRE-084, a selective and reference s 1 receptor agonist, and xanomeline, a muscarinic ligand presenting similar profile as ANAVEX2-73 on M1 and M2 subtypes, confirmed that both muscarinic and s 1 targets are involved in the ANAVEX2-73 effects. The drug, acting synergistically on both targets, but with moderate affinity, presents a promising pharmacological profile.

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Section: A Gsk-3b Inhibitor Alleviates Ab 25-35 -Induced Toxicity Andmentioning

confidence: 91%

Blockade of Tau Hyperphosphorylation and Aβ1–42 Generation by the Aminotetrahydrofuran Derivative ANAVEX2-73, a Mixed Muscarinic and σ1 Receptor Agonist, in a Nontransgenic Mouse Model of Alzheimer’s Disease

Lahmy

Meunier²,

Malmström³

et al. 2013

Neuropsychopharmacol

134

View full text Add to dashboard Cite

show abstract

“…By contrast, the trial in amnestic mild cognitive impairment suggested that lithium treatment was associated with a decrease in p-tau in the CSF and better cognitive performance. Another GSK inhibitor, 2-methyl-5-(3-{4-[(S)-methylsulfinyl] phenyl}-1-benzofuran-5-yl)-1,3,4-oxadiazole, reduces hippocampal tau phosphorylation at GSK-3 sites and ameliorates behavioural dysfunction in 3×Tg-AD mice 70. The non-specific tau kinase inhibitor K252a (for CDK5, GSK3 and ERK1) also reduced levels of hyperphosphorylated tau and ameliorated the motor phenotype in P301L mutant tau Tg mice (JNPL3) 71.…”

Section: Therapeutic Strategies For Tau Mediated Neurodegenerationmentioning

confidence: 99%

Therapeutic strategies for tau mediated neurodegeneration

Yoshiyama

Lee

Trojanowski

2012

J Neurol Neurosurg Psychiatry

114

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Based on the amyloid hypothesis, controlling β-amyloid protein (Aβ) accumulation is supposed to suppress downstream pathological events, tau accumulation, neurodegeneration and cognitive decline. However, in recent clinical trials, Aβ removal or reducing Aβ production has shown limited efficacy. Moreover, while active immunisation with Aβ resulted in the clearance of Aβ, it did not prevent tau pathology or neurodegeneration. This prompts the concern that it might be too late to employ Aβ targeting therapies once tau mediated neurodegeneration has occurred. Therefore, it is timely and very important to develop tau directed therapies. The pathomechanisms of tau mediated neurodegeneration are unclear but hyperphosphorylation, oligomerisation, fibrillisation and propagation of tau pathology have been proposed as the likely pathological processes that induce loss of function or gain of toxic function of tau, causing neurodegeneration. Here we review the strategies for tau directed treatments based on recent progress in research on tau and our understanding of the pathomechanisms of tau mediated neurodegeneration.

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“…However, the mice did not live longer. 2-Methyl-5-(3-{4-[(S)-methylsulfinyl]phenyl}-1-benzofuran-5-yl)-1,3,4-oxadiazole, another novel GSK-3 inhibitor, has recently been reported to produce a similar positive outcome in vitro and in a mouse model (Onishi et al, 2011). Successfully targeting GSK-3, now a goal in many disease fields, is evidently a complex undertaking.…”

Section: F Glycogen Synthase Kinase-3 Antagonistsmentioning

confidence: 99%

“…Surprisingly, A␤ plaque removal was the only mechanism considered by these authors, despite the doubt cast on the utility of this endpoint by the AD patient trial of AN1792 (A␤42; Elan Pharmaceuticals, South San Francisco, CA) several years ago (Holmes et al, 2008). It is useful to recall, when interpreting Onishi et al, 2011 this bexarotene data, that anti-TNF treatment produces a very similar outcome in the same mouse model (Shi et al, 2011), and an apoE mimetic has since done so in a related mouse strain (Vitek et al, 2012). Literature exists on the side effects of bexarotene, but whether these arise from high apoE or other consequences of retinoid X receptor activation has yet to be determined.…”

Section: H Apolipoprotein E Mimetics and Bexarotenementioning

confidence: 99%

Tumor Necrosis Factor-Induced Cerebral Insulin Resistance in Alzheimer's Disease Links Numerous Treatment Rationales

et al. 2012

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A novel glycogen synthase kinase‐3 inhibitor 2‐methyl‐5‐(3‐{4‐[(S )‐methylsulfinyl]phenyl}‐1‐benzofuran‐5‐yl)‐1,3,4‐oxadiazole decreases tau phosphorylation and ameliorates cognitive deficits in a transgenic model of Alzheimer’s disease

Cited by 79 publications

References 50 publications

Blockade of Tau Hyperphosphorylation and Aβ1–42 Generation by the Aminotetrahydrofuran Derivative ANAVEX2-73, a Mixed Muscarinic and σ1 Receptor Agonist, in a Nontransgenic Mouse Model of Alzheimer’s Disease

Blockade of Tau Hyperphosphorylation and Aβ1–42 Generation by the Aminotetrahydrofuran Derivative ANAVEX2-73, a Mixed Muscarinic and σ1 Receptor Agonist, in a Nontransgenic Mouse Model of Alzheimer’s Disease

Therapeutic strategies for tau mediated neurodegeneration

Tumor Necrosis Factor-Induced Cerebral Insulin Resistance in Alzheimer's Disease Links Numerous Treatment Rationales

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