Relationship of the extended tau haplotype to tau biochemistry and neuropathology in progressive supranuclear palsy

Liu, Wan Kyng; Le, Tien V.; Adamson, Jennifer; Baker, Matthew; Cookson, Natalie; Hardy, John; Hutton, Michael; Yen, Shu Hui; Dickson, Dennis W.

doi:10.1002/ana.1159

Cited by 70 publications

(33 citation statements)

References 38 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Previous studies have identified a strong association between the dinucleotide repeat polymorphism A0 and the risk of PSP, CBD and FTD [11 -13]. Remarkably, reports in PSP have shown no relation of the A0/A0 genotype to the biochemical characteristics such as tau deposit composition or to the clinical phenotype [14]. Also in ALS, we found no association of the A0/A0 genotype with the age and site of disease onset or the presence of dementia.…”

Section: Discussioncontrasting

confidence: 74%

Frequency of a tau genotype in amyotrophic lateral sclerosis

Münch

Prechter

et al. 2005

Journal of the Neurological Sciences

View full text Add to dashboard Cite

Section: Discussioncontrasting

confidence: 74%

Frequency of a tau genotype in amyotrophic lateral sclerosis

Münch

Prechter

et al. 2005

Journal of the Neurological Sciences

View full text Add to dashboard Cite

“…Specifically, this group of diseases may include PSP, CBD, argyrophilic grain disease, and other FTDP-17 diseases resulting from exon 10 splicing mutations (Mailliot et al, 1998;Sergeant et al, 1999;Arai et al, 2001;Liu et al, 2001;Katsuse et al, 2003;Morris et al, 2003). These tauopathies all have similar characteristics of astrocytic and neuronal tau accumulation, predominantly 4R insoluble tau and motor and cognitive deficits.…”

Section: Discussionmentioning

confidence: 99%

The Tau N279K Exon 10 Splicing Mutation Recapitulates Frontotemporal Dementia and Parkinsonism Linked to Chromosome 17 Tauopathy in a Mouse Model

Dawson¹,

Cantillana²,

Chen³

et al. 2007

J. Neurosci.

View full text Add to dashboard Cite

Intracellular tau deposits are characteristic of several neurodegenerative disorders called tauopathies. The tau protein regulates the stability and assembly of microtubules by binding to microtubules through three or four microtubule-binding repeats (3R and 4R). The number of microtubule-binding repeats is determined by the inclusion or exclusion of the second microtubule-binding repeat encoded by exon 10 of the TAU gene. TAU gene mutations that alter the inclusion of exon 10, and hence the 4R:3R ratio, are causal in the tauopathy frontotemporal dementia and parkinsonism linked to chromosome 17 (FTDP-17). A mutation located in exon 10 has been identified in several FTDP-17 families that present with increased exon 10 inclusion in both mRNA and protein, parkinsonism, movement disorders, and dementia. We have engineered a human tau minigene construct that was designed to allow alternative splicing of the tau exon 10. Here we demonstrate that transgenic mice expressing human tau protein with this mutation develop neurodegeneration as result of aberrant splicing. The mice recapitulate many of the disease hallmarks that are seen in patients with this mutation, including increased tau exon 10 inclusion in both mRNA and protein, motor and behavioral deficits, and tau protein accumulation in neurons and tufted astrocytes. Furthermore, these mice present with degeneration of the nigrostriatal dopaminergic pathway, suggesting a possible mechanism for parkinsonism in FTDP-17. Additionally, activated caspase-3 immunoreactivity in both neurons and astrocytes implicates the involvement of the apoptotic pathway in the pathology of these mice.

show abstract

“…All blots were incubated with a blocking solution containing 5% nonfat milk, 0.1% goat serum and 0.1% Tween-20 in TBS, incubated with various antibodies, and washed as previously described. 5,9,33 The washed blots were incubated for 1 hour at room temperature with peroxidase-conjugated, goat anti-rabbit (1:4000, Chemicon, Temecula, CA), anti-mouse IgG (1:2000, Bio Rad, Hercules, CA), followed with washing and detection of bound antibodies with the enhanced chemiluminescence system (ECL plus; Amersham Biosciences, Piscataway, NJ). Immunoreactivity of GSK3 proteins was analyzed from scanned films using MCID software (Imaging Research Inc., Ontario, Canada).…”

Section: Western Blottingmentioning

confidence: 99%

Co-Localization of Glycogen Synthase Kinase-3 with Neurofibrillary Tangles and Granulovacuolar Degeneration in Transgenic Mice

Ishizawa

Sahara

Ishiguro

et al. 2003

The American Journal of Pathology

Self Cite

View full text Add to dashboard Cite

Transgenic mice expressing human tau with P301L missense mutation (JNPL3) develop progressive amyotrophy, neurofibrillary degeneration, and neuronal loss. Mating of JNPL3 with transgenic mice expressing mutant amyloid precursor protein (Tg2576) leads to bigenic (TAPP) mice with enhanced neurofibrillary pathology. TAPP and JNPL3 mice were studied with immunocytochemistry and immunoblotting with antibodies to glycogen synthase kinase-3 (GKS3) to determine whether the development of tauopathy is associated with activation or increased expression of GSK3, and when the observed changes occur with respect to neurofibrillary tangle (NFT) formation. Accumulation of GSK3␣/␤ phosphorylated at Y279/216 was observed in neurons containing NFTs and granulovacuolar degeneration (GVD), but not in normal neurons or neurons with pretangles. More GSK3 immunoreactive NFTs were detected in TAPP than JNPL3 mice, especially in the amygdala. These differences were notable only in old animals. There was no significant difference between animals with and without NFTs in the level of total, inactive, or Y216-phosphorylated (pY216)GSK3␤. No apparent GSK3 accumulation was detected in neurons in Tg2576 mice. There was also no significant difference in the distribution of GSK3 in lysates fractionated based on their solubility in various reagents, including the sarkosyl-insoluble fraction. The results suggest that the pY216 GSK3␤ accumulates in NFT and GVD due to redistribution rather than increased expression or activation, and that pre-existence of tau abnormalities is required for APP/A␤ to exert their effects on tau pathology in TAPP mice. Neurofibrillary tangles (NFTs) and senile plaques are the two major histopathological lesions in Alzheimer's disease (AD). NFTs are composed of polymerized microtubule-associated protein tau.1 Neurofibrillary lesions are also prominent features of progressive supranuclear palsy, corticobasal degeneration, Pick's disease and frontotemporal dementia and parkinsonism linked to chromosome 17 (FTDP17), which together are referred to as the tauopathies.2 Several lines of transgenic mice have recently been generated that express wild-type or mutant human tau, and have been shown to develop tau abnormalities similar to those observed in humans. [3][4][5][6][7][8] Among them, mice expressing human four-repeat tau with no amino-terminal inserts (4R0N) and with P301L or with P301S mutation display robust neurofibrillary pathology. 5,8 In mice expressing P301L tau (referred to as JNPL3 mice), abnormal accumulation of tau is detected at as early as 3 months of age.5 Most of the abnormal tau immunoreactive neurons are negative with Gallyas silver stain and are considered to be pretangles. As animals age, the number of Gallyas-positive NFT neurons increases. These NFTs were shown by immunoelectron microscopy to contain bundles of filamentous tau.5 NFTs in JNPL3 mice were detected earlier in spinal cord than brain and were accompanied by a decrease in tau solubility characterized by resistance to extraction in detergent...

show abstract

Relationship of the extended tau haplotype to tau biochemistry and neuropathology in progressive supranuclear palsy

Cited by 70 publications

References 38 publications

Frequency of a tau genotype in amyotrophic lateral sclerosis

Frequency of a tau genotype in amyotrophic lateral sclerosis

The Tau N279K Exon 10 Splicing Mutation Recapitulates Frontotemporal Dementia and Parkinsonism Linked to Chromosome 17 Tauopathy in a Mouse Model

Co-Localization of Glycogen Synthase Kinase-3 with Neurofibrillary Tangles and Granulovacuolar Degeneration in Transgenic Mice

Contact Info

Product

Resources

About