27 results on '"Sydow, Astrid"'
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2. Functional networks are impaired by elevated tau-protein but reversible in a regulatable Alzheimer’s disease mouse model
3. Reversal of Tau-Dependent Cognitive Decay by Blocking Adenosine A1 Receptors: Comparison of Transgenic Mouse Models with Different Levels of Tauopathy
4. The Tau/A152T mutation, a risk factor for frontotemporal‐spectrum disorders, leads to NR2B receptor‐mediated excitotoxicity
5. Reversal of tau-dependent cognitive decay by blocking adenosine A1 receptors in mouse models of tauopathy
6. Cognitive defects are reversible in inducible mice expressing pro-aggregant full-length human Tau
7. Reversibility of Tau-Related Cognitive Defects in a Regulatable FTD Mouse Model
8. A zebrafish model of tauopathy allows in vivo imaging of neuronal cell death and drug evaluation
9. Regulatable transgenic mouse models of Alzheimer disease: onset, reversibility and spreading of Tau pathology
10. The Tau/Ala152Thr mutation, a risk factor for frontotemporal-spectrum disorders, leads to neuroinflammation, cognitive decline and NR2B receptor-mediated excitotoxicity in a novel transgenic mouse model
11. Additional file 1: of Age-dependent neuroinflammation and cognitive decline in a novel Ala152Thr-Tau transgenic mouse model of PSP and AD
12. W04-02: Tau toxicity and rescue in cell and animal models of tau pathology
13. Adenosine A 1 receptor antagonist rolofylline alleviates axonopathy caused by human Tau ΔK280
14. The Tau/A152T mutation, a risk factor for frontotemporal‐spectrum disorders, leads to NR 2B receptor‐mediated excitotoxicity
15. Tau, axonal transport and Alzheimer's disease
16. Age-dependent neuroinflammation and cognitive decline in a novel Ala152Thr-Tau transgenic mouse model of PSP and AD
17. Preventive methylene blue treatment preserves cognition in mice expressing full-length pro-aggregant human Tau
18. Pro-aggregant Tau impairs mossy fiber plasticity due to structural changes and Ca++ dysregulation
19. Adenosine A1 receptor antagonist rolofylline alleviates axonopathy caused by human Tau ΔK280.
20. O3-04-02: Cognitive decline and defects in neuroplasticity are reversible in an inducible mouse model expressing pro-aggregant full-length human tau
21. Tau-Induced Defects in Synaptic Plasticity, Learning, and Memory Are Reversible in Transgenic Mice after Switching Off the Toxic Tau Mutant
22. O4-05-02: Tau-induced defects in hippocampal neuroplasticity, learning and memory are reversible in a regulatable transgenic mouse model
23. ‘Prion-Like’ Propagation of Mouse and Human Tau Aggregates in an Inducible Mouse Model of Tauopathy
24. Pro-aggregant Tau impairs mossy fiber plasticity due to structural changes and Ca++ dysregulation.
25. Cognitive defects are reversible in inducible mice expressing pro-aggregant full-length human Tau.
26. Cognitive decline and defects in neuroplasticity are reversible in an inducible mouse model expressing pro-aggregant full-length human tau
27. Tau-induced defects in hippocampal neuroplasticity, learning and memory are reversible in a regulatable transgenic mouse model
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