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1. Alzheimer's disease associated isoforms of human CD33 distinctively modulate microglial cell responses in 5XFAD mice.

2. Application of N-Terminal Labeling Methods Provide Novel Insights into Endoproteolysis of the Prion Protein in Vivo .

3. Microglial APOE4: more is less and less is more.

4. CD33 isoforms in microglia and Alzheimer's disease: Friend and foe.

5. Streamlined high-throughput cloning protocol to generate arrayed mutant libraries.

6. Beta-endoproteolysis of the cellular prion protein by dipeptidyl peptidase-4 and fibroblast activation protein.

7. Increasing phagocytosis of microglia by targeting CD33 with liposomes displaying glycan ligands.

8. The CD33 short isoform is a gain-of-function variant that enhances Aβ 1-42 phagocytosis in microglia.

10. Quaternary Structure Changes for PrP Sc Predate PrP C Downregulation and Neuronal Death During Progression of Experimental Scrapie Disease.

11. Cellular Biology of Tau Diversity and Pathogenic Conformers.

12. Metabolomic study of disease progression in scrapie prion infected mice; validation of a novel method for brain metabolite extraction.

13. Diverse, evolving conformer populations drive distinct phenotypes in frontotemporal lobar degeneration caused by the same MAPT-P301L mutation.

14. The CNS in inbred transgenic models of 4-repeat Tauopathy develops consistent tau seeding capacity yet focal and diverse patterns of protein deposition.

15. Microtubule Dynamicity Is More Important than Stability in Memory Formation: an In Vivo Study.

16. Chronic, long-term social stress can cause decreased microtubule protein network activity and dynamics in cerebral cortex of male Wistar rats.

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