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Literature DB >> 19363289

A zebrafish model of tauopathy allows in vivo imaging of neuronal cell death and drug evaluation.

Dominik Paquet¹, Ratan Bhat, Astrid Sydow, Eva-Maria Mandelkow, Stefan Berg, Sven Hellberg, Johanna Fälting, Martin Distel, Reinhard W Köster, Bettina Schmid, Christian Haass.

Abstract

Our aging society is confronted with a dramatic increase of patients suffering from tauopathies, which include Alzheimer disease and certain frontotemporal dementias. These disorders are characterized by typical neuropathological lesions including hyperphosphorylation and subsequent aggregation of TAU protein and neuronal cell death. Currently, no mechanism-based cures are available. We generated fluorescently labeled TAU transgenic zebrafish, which rapidly recapitulated key pathological features of tauopathies, including phosphorylation and conformational changes of human TAU protein, tangle formation, neuronal and behavioral disturbances, and cell death. Due to their optical transparency and small size, zebrafish larvae are well suited for both in vivo imaging and drug development. TAU-induced neuronal cell death was imaged by time-lapse microscopy in vivo. Furthermore, we used this zebrafish model to identify compounds targeting the TAU kinase glycogen synthase kinase 3beta (GSK3beta). We identified a newly developed highly active GSK3beta inhibitor, AR-534, by rational drug design. AR-534 reduced TAU phosphorylation in TAU transgenic zebrafish. This transgenic zebrafish model may become a valuable tool for further studies of the neuropathology of dementia.

Entities: Chemical Disease Gene Species

Mesh：

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Year: 2009 PMID： 19363289 PMCID： PMC2673864 DOI： 10.1172/JCI37537

Source DB: PubMed Journal: J Clin Invest ISSN： 0021-9738 Impact factor: 14.808

45 in total

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Journal: Adv Drug Deliv Rev Date: 1999-04-05 Impact factor: 15.470

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3. GATEWAY recombinational cloning: application to the cloning of large numbers of open reading frames or ORFeomes.

Authors: A J Walhout; G F Temple; M A Brasch; J L Hartley; M A Lorson; S van den Heuvel; M Vidal
Journal: Methods Enzymol Date: 2000 Impact factor: 1.600

Review 4. GSK-3: tricks of the trade for a multi-tasking kinase.

Authors: Bradley W Doble; James R Woodgett
Journal: J Cell Sci Date: 2003-04-01 Impact factor: 5.285

5. A gamma-secretase inhibitor blocks Notch signaling in vivo and causes a severe neurogenic phenotype in zebrafish.

Authors: Andrea Geling; Harald Steiner; Michael Willem; Laure Bally-Cuif; Christian Haass
Journal: EMBO Rep Date: 2002-07 Impact factor: 8.807

6. Functional dissection of the Tol2 transposable element identified the minimal cis-sequence and a highly repetitive sequence in the subterminal region essential for transposition.

Authors: Akihiro Urasaki; Ghislaine Morvan; Koichi Kawakami
Journal: Genetics Date: 2006-09-07 Impact factor: 4.562

7. Lithium reduces tau phosphorylation by inhibition of glycogen synthase kinase-3.

Authors: M Hong; D C Chen; P S Klein; V M Lee
Journal: J Biol Chem Date: 1997-10-03 Impact factor: 5.157

8. Organization of hindbrain segments in the zebrafish embryo.

Authors: B Trevarrow; D L Marks; C B Kimmel
Journal: Neuron Date: 1990-05 Impact factor: 17.173

9. Missorting of tau in neurons causes degeneration of synapses that can be rescued by the kinase MARK2/Par-1.

Authors: Edda Thies; Eva-Maria Mandelkow
Journal: J Neurosci Date: 2007-03-14 Impact factor: 6.167

10. Epitope mapping of monoclonal antibodies to the paired helical filaments of Alzheimer's disease: identification of phosphorylation sites in tau protein.

Authors: M Goedert; R Jakes; R A Crowther; P Cohen; E Vanmechelen; M Vandermeeren; P Cras
Journal: Biochem J Date: 1994-08-01 Impact factor: 3.857

90 in total

Review 1. Modeling human neurodegenerative diseases in transgenic systems.

Authors: Miguel A Gama Sosa; Rita De Gasperi; Gregory A Elder
Journal: Hum Genet Date: 2011-12-14 Impact factor: 4.132

2. NFAT/Fas signaling mediates the neuronal apoptosis and motor side effects of GSK-3 inhibition in a mouse model of lithium therapy.

Authors: Raquel Gómez-Sintes; José J Lucas
Journal: J Clin Invest Date: 2010-06-07 Impact factor: 14.808

A zebrafish model of tauopathy allows in vivo imaging of neuronal cell death and drug evaluation.

1. In vitro model for evaluating drug transport across the blood-brain barrier.

2. Analysis of upstream elements in the HuC promoter leads to the establishment of transgenic zebrafish with fluorescent neurons.

3. GATEWAY recombinational cloning: application to the cloning of large numbers of open reading frames or ORFeomes.

Review 4. GSK-3: tricks of the trade for a multi-tasking kinase.

5. A gamma-secretase inhibitor blocks Notch signaling in vivo and causes a severe neurogenic phenotype in zebrafish.

6. Functional dissection of the Tol2 transposable element identified the minimal cis-sequence and a highly repetitive sequence in the subterminal region essential for transposition.

7. Lithium reduces tau phosphorylation by inhibition of glycogen synthase kinase-3.

8. Organization of hindbrain segments in the zebrafish embryo.

9. Missorting of tau in neurons causes degeneration of synapses that can be rescued by the kinase MARK2/Par-1.

10. Epitope mapping of monoclonal antibodies to the paired helical filaments of Alzheimer's disease: identification of phosphorylation sites in tau protein.

Review 1. Modeling human neurodegenerative diseases in transgenic systems.

2. NFAT/Fas signaling mediates the neuronal apoptosis and motor side effects of GSK-3 inhibition in a mouse model of lithium therapy.

3. Morphofunctional changes in goldfish Mauthner neurons after application of beta-amyloid.

4. Initiation and propagation of neurodegeneration.

5. A novel approach to study motor neurons from zebrafish embryos and larvae in culture.

Review 6. Animal models in the drug discovery pipeline for Alzheimer's disease.

7. Can zebrafish be used as animal model to study Alzheimer's disease?

8. Role of a ubiquitously expressed receptor in the vertebrate olfactory system.

9. Evaluation of Improved Glycogen Synthase Kinase-3α Inhibitors in Models of Acute Myeloid Leukemia.

10. Genetically modified species in research: Opportunities and challenges for the histology core laboratory.