The potential for beta-structure in the repeat domain of tau protein determines aggregation, synaptic decay, neuronal loss, and coassembly with endogenous Tau in inducible mouse models of tauopathy.

Maria-Magdalena Mocanu; Astrid Nissen; Katrin Eckermann; Inna Khlistunova; Jacek Biernat; Dagmar Drexler; Olga Petrova; Kai Schönig; Hermann Bujard; Eckhard Mandelkow; Lepu Zhou; Gabriele M. Rune; Eva-Maria Mandelkow

The potential for beta-structure in the repeat domain of tau protein determines aggregation, synaptic decay, neuronal loss, and coassembly with endogenous Tau in inducible mouse models of tauopathy.

Standard

The potential for beta-structure in the repeat domain of tau protein determines aggregation, synaptic decay, neuronal loss, and coassembly with endogenous Tau in inducible mouse models of tauopathy. / Mocanu, Maria-Magdalena; Nissen, Astrid; Eckermann, Katrin; Khlistunova, Inna; Biernat, Jacek; Drexler, Dagmar; Petrova, Olga; Schönig, Kai; Bujard, Hermann; Mandelkow, Eckhard; Zhou, Lepu; Rune, Gabriele M.; Mandelkow, Eva-Maria.

in: J NEUROSCI, Jahrgang 28, Nr. 3, 3, 2008, S. 737-748.

Publikationen: SCORING: Beitrag in Fachzeitschrift/Zeitung › SCORING: Zeitschriftenaufsatz › Forschung › Begutachtung

Harvard

Mocanu, M-M, Nissen, A, Eckermann, K, Khlistunova, I, Biernat, J, Drexler, D, Petrova, O, Schönig, K, Bujard, H, Mandelkow, E, Zhou, L, Rune, GM & Mandelkow, E-M 2008, 'The potential for beta-structure in the repeat domain of tau protein determines aggregation, synaptic decay, neuronal loss, and coassembly with endogenous Tau in inducible mouse models of tauopathy.', J NEUROSCI, Jg. 28, Nr. 3, 3, S. 737-748. <http://www.ncbi.nlm.nih.gov/pubmed/18199773?dopt=Citation>

APA

Mocanu, M-M., Nissen, A., Eckermann, K., Khlistunova, I., Biernat, J., Drexler, D., Petrova, O., Schönig, K., Bujard, H., Mandelkow, E., Zhou, L., Rune, G. M., & Mandelkow, E-M. (2008). The potential for beta-structure in the repeat domain of tau protein determines aggregation, synaptic decay, neuronal loss, and coassembly with endogenous Tau in inducible mouse models of tauopathy. J NEUROSCI, 28(3), 737-748. [3]. http://www.ncbi.nlm.nih.gov/pubmed/18199773?dopt=Citation

Vancouver

Mocanu M-M, Nissen A, Eckermann K, Khlistunova I, Biernat J, Drexler D et al. The potential for beta-structure in the repeat domain of tau protein determines aggregation, synaptic decay, neuronal loss, and coassembly with endogenous Tau in inducible mouse models of tauopathy. J NEUROSCI. 2008;28(3):737-748. 3.

Bibtex

@article{c5f637bf436d4e0e91406bef2f2b5c5d,

title = "The potential for beta-structure in the repeat domain of tau protein determines aggregation, synaptic decay, neuronal loss, and coassembly with endogenous Tau in inducible mouse models of tauopathy.",

abstract = "We describe two new transgenic mouse lines for studying pathological changes of Tau protein related to Alzheimer's disease. They are based on the regulatable expression of the four-repeat domain of human Tau carrying the FTDP17 (frontotemporal dementia and parkinsonism linked to chromosome 17) mutation deltaK280 (Tau(RD)/deltaK280), or the deltaK280 plus two proline mutations in the hexapeptide motifs (Tau(RD)/deltaK280/I277P/I308P). The deltaK280 mutation accelerates aggregation ({"}proaggregation mutant{"}), whereas the proline mutations inhibit Tau aggregation in vitro and in cell models ({"}antiaggregation mutant{"}). The inducible transgene expression was driven by the forebrain-specific CaMKIIalpha (calcium/calmodulin-dependent protein kinase IIalpha) promoter. The proaggregation mutant leads to Tau aggregates and tangles as early as 2-3 months after gene expression, even at low expression (70% of endogenous mouse Tau). The antiaggregation mutant does not aggregate even after 22 months of gene expression. Both mutants show missorting of Tau in the somatodendritic compartment and hyperphosphorylation in the repeat domain [KXGS motifs, targets of the kinase MARK (microtubule affinity regulating kinase)]. This indicates that these changes are related to Tau expression rather than aggregation. The proaggregation mutant causes astrogliosis, loss of synapses and neurons from 5 months of gene expression onward, arguing that Tau toxicity is related to aggregation. Remarkably, the human proaggregation mutant Tau(RD) coaggregates with mouse Tau, coupled with missorting and hyperphosphorylation at multiple sites. When expression of proaggregation Tau(RD) is switched off, soluble and aggregated exogenous Tau(RD) disappears within 1.5 months. However, tangles of mouse Tau, hyperphosphorylation, and missorting remain, suggesting an extended lifetime of aggregated wild-type Tau once a pathological conformation and aggregation is induced by a proaggregation Tau species.",

author = "Maria-Magdalena Mocanu and Astrid Nissen and Katrin Eckermann and Inna Khlistunova and Jacek Biernat and Dagmar Drexler and Olga Petrova and Kai Sch{\"o}nig and Hermann Bujard and Eckhard Mandelkow and Lepu Zhou and Rune, {Gabriele M.} and Eva-Maria Mandelkow",

year = "2008",

language = "Deutsch",

volume = "28",

pages = "737--748",

journal = "J NEUROSCI",

issn = "0270-6474",

publisher = "Society for Neuroscience",

number = "3",

}

RIS

TY - JOUR

T1 - The potential for beta-structure in the repeat domain of tau protein determines aggregation, synaptic decay, neuronal loss, and coassembly with endogenous Tau in inducible mouse models of tauopathy.

AU - Mocanu, Maria-Magdalena

AU - Nissen, Astrid

AU - Eckermann, Katrin

AU - Khlistunova, Inna

AU - Biernat, Jacek

AU - Drexler, Dagmar

AU - Petrova, Olga

AU - Schönig, Kai

AU - Bujard, Hermann

AU - Mandelkow, Eckhard

AU - Zhou, Lepu

AU - Rune, Gabriele M.

AU - Mandelkow, Eva-Maria

PY - 2008

Y1 - 2008

N2 - We describe two new transgenic mouse lines for studying pathological changes of Tau protein related to Alzheimer's disease. They are based on the regulatable expression of the four-repeat domain of human Tau carrying the FTDP17 (frontotemporal dementia and parkinsonism linked to chromosome 17) mutation deltaK280 (Tau(RD)/deltaK280), or the deltaK280 plus two proline mutations in the hexapeptide motifs (Tau(RD)/deltaK280/I277P/I308P). The deltaK280 mutation accelerates aggregation ("proaggregation mutant"), whereas the proline mutations inhibit Tau aggregation in vitro and in cell models ("antiaggregation mutant"). The inducible transgene expression was driven by the forebrain-specific CaMKIIalpha (calcium/calmodulin-dependent protein kinase IIalpha) promoter. The proaggregation mutant leads to Tau aggregates and tangles as early as 2-3 months after gene expression, even at low expression (70% of endogenous mouse Tau). The antiaggregation mutant does not aggregate even after 22 months of gene expression. Both mutants show missorting of Tau in the somatodendritic compartment and hyperphosphorylation in the repeat domain [KXGS motifs, targets of the kinase MARK (microtubule affinity regulating kinase)]. This indicates that these changes are related to Tau expression rather than aggregation. The proaggregation mutant causes astrogliosis, loss of synapses and neurons from 5 months of gene expression onward, arguing that Tau toxicity is related to aggregation. Remarkably, the human proaggregation mutant Tau(RD) coaggregates with mouse Tau, coupled with missorting and hyperphosphorylation at multiple sites. When expression of proaggregation Tau(RD) is switched off, soluble and aggregated exogenous Tau(RD) disappears within 1.5 months. However, tangles of mouse Tau, hyperphosphorylation, and missorting remain, suggesting an extended lifetime of aggregated wild-type Tau once a pathological conformation and aggregation is induced by a proaggregation Tau species.

AB - We describe two new transgenic mouse lines for studying pathological changes of Tau protein related to Alzheimer's disease. They are based on the regulatable expression of the four-repeat domain of human Tau carrying the FTDP17 (frontotemporal dementia and parkinsonism linked to chromosome 17) mutation deltaK280 (Tau(RD)/deltaK280), or the deltaK280 plus two proline mutations in the hexapeptide motifs (Tau(RD)/deltaK280/I277P/I308P). The deltaK280 mutation accelerates aggregation ("proaggregation mutant"), whereas the proline mutations inhibit Tau aggregation in vitro and in cell models ("antiaggregation mutant"). The inducible transgene expression was driven by the forebrain-specific CaMKIIalpha (calcium/calmodulin-dependent protein kinase IIalpha) promoter. The proaggregation mutant leads to Tau aggregates and tangles as early as 2-3 months after gene expression, even at low expression (70% of endogenous mouse Tau). The antiaggregation mutant does not aggregate even after 22 months of gene expression. Both mutants show missorting of Tau in the somatodendritic compartment and hyperphosphorylation in the repeat domain [KXGS motifs, targets of the kinase MARK (microtubule affinity regulating kinase)]. This indicates that these changes are related to Tau expression rather than aggregation. The proaggregation mutant causes astrogliosis, loss of synapses and neurons from 5 months of gene expression onward, arguing that Tau toxicity is related to aggregation. Remarkably, the human proaggregation mutant Tau(RD) coaggregates with mouse Tau, coupled with missorting and hyperphosphorylation at multiple sites. When expression of proaggregation Tau(RD) is switched off, soluble and aggregated exogenous Tau(RD) disappears within 1.5 months. However, tangles of mouse Tau, hyperphosphorylation, and missorting remain, suggesting an extended lifetime of aggregated wild-type Tau once a pathological conformation and aggregation is induced by a proaggregation Tau species.

M3 - SCORING: Zeitschriftenaufsatz

VL - 28

SP - 737

EP - 748

JO - J NEUROSCI

JF - J NEUROSCI

SN - 0270-6474

IS - 3

M1 - 3

ER -