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1. Novel App knock-in mouse model shows key features of amyloid pathology and reveals profound metabolic dysregulation of microglia

2. The role of microglia in processing and spreading of bioactive tau seeds in Alzheimer’s disease

3. Synaptic Tau Seeding Precedes Tau Pathology in Human Alzheimer's Disease Brain

4. Lysosomal functions of progranulin and implications for treatment of frontotemporal dementia

5. Targeting Transferrin Receptor to Transport Antisense Oligonucleotides Across the Blood-Brain Barrier

6. Rate‐limiting processes of tau aggregate accumulation in Alzheimer's disease

7. Rescue of a lysosomal storage disorder caused by Grn loss-of-function with a brain penetrant progranulin biologic

8. Current directions in tau research: Highlights from Tau 2020

9. Pathogenic tau accelerates aging-associated activation of transposable elements in the mouse central nervous system

10. Fibrillar Aβ causes profound microglial metabolic perturbations in a novel APP knock-in mouse model

11. Persistent repression of tau in the brain using engineered zinc finger protein transcription factors

12. A brain penetrant progranulin biotherapeutic rescues lysosomal and inflammatory phenotypes in the brain of GRN knockout mice

13. Amplification, not spreading limits rate of tau aggregate accumulation in Alzheimer’s disease

14. Brain delivery of therapeutic proteins using an Fc fragment blood-brain barrier transport vehicle in mice and monkeys

15. Pathological correlations of [F-18]-AV-1451 imaging in non-alzheimer tauopathies

16. Increased 4R-Tau Induces Pathological Changes in a Human-Tau Mouse Model

17. Tau protein disrupts nucleocytoplasmic transport in Alzheimer’s disease

18. Tau reduction in the presence of amyloid-β prevents tau pathology and neuronal death in vivo

19. Tau Protein Disrupts Nucleocytoplasmic Transport in Alzheimerrs Disease

20. Enhanced Tau Aggregation in the Presence of Amyloid β

21. Tau Antibody Targeting Pathological Species Blocks Neuronal Uptake and Interneuron Propagation of Tau in Vitro

22. Tau at the Crossroads between Neurotoxicity and Neuroprotection

23. Antisense Reduction of Tau in Adult Mice Protects against Seizures

24. Antisense Oligonucleotides: Treating Neurodegeneration at the Level of RNA

25. Transcriptional Coactivators Are Not Required for Herpes Simplex Virus Type 1 Immediate-Early Gene Expression In Vitro

26. Seed-competent high-molecular-weight tau species accumulates in the cerebrospinal fluid of Alzheimer's disease mouse model and human patients

27. Removing endogenous tau does not prevent tau propagation yet reduces its neurotoxicity

28. Tau reduction prevents neuronal loss and reverses pathological tau deposition and seeding in mice with tauopathy

29. O2‐06‐01: Lack of endogenous tau permits tau spreading and protects against tau toxicity in transgenic mice

30. O3‐04‐03: Tau splicing in vivo : Application in mouse models of tauopathy confers functional and pathological changes

31. P3‐071: A unique high‐molecular‐weight tau species is involved in propagation and accumulates in the cerebrospinal fluid of Alzheimer's disease patients

32. Neuronal uptake and propagation of a rare phosphorylated high-molecular-weight tau derived from Alzheimer's disease brain

33. Characterization of TauC3 antibody and demonstration of its potential to block tau propagation

34. Distinct tau prion strains propagate in cells and mice and define different tauopathies

35. Heparan sulfate proteoglycans mediate internalization and propagation of specific proteopathic seeds

36. P1‐286: Using antisense oligonucleotides to knockdown endogenous brain tau in vivo

37. Implicating Calpain in Tau-Mediated Toxicity In Vivo

38. In vivo rate-determining steps of tau seed accumulation in Alzheimer’s disease

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