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1. A novel D-amino acid peptide with therapeutic potential (ISAD1) inhibits aggregation of neurotoxic disease-relevant mutant Tau and prevents Tau toxicity in vitro

2. Reversal of Tau-Dependent Cognitive Decay by Blocking Adenosine A1 Receptors: Comparison of Transgenic Mouse Models with Different Levels of Tauopathy

3. FRET-based Tau seeding assay does not represent prion-like templated assembly of Tau filaments

4. Novel antibody against low‐n oligomers of tau protein promotes clearance of tau in cells via lysosomes

5. The Plasma Factor XIII Heterotetrameric Complex Structure: Unexpected Unequal Pairing within a Symmetric Complex

6. Disruption of Structural Disulfides of Coagulation FXIII-B Subunit; Functional Implications for a Rare Bleeding Disorder

7. Microfluidic Chamber Technology to Study Missorting and Spreading of Tau Protein in Alzheimer's Disease

8. A combinatorial native MS and LC-MS/MS approach reveals high intrinsic phosphorylation of human Tau but minimal levels of other key modifications

9. Reversal of tau-dependent cognitive decay by blocking adenosine A1 receptors in mouse models of tauopathy

10. Molecular crowding and RNA synergize to promote phase separation, microtubule interaction, and seeding of Tau condensates

13. Spreading of Tau Protein Does Not Depend on Aggregation Propensity

14. FRET-based Tau seeding assay does not represent prion-like templated assembly of Tau filaments

15. Novel antibody against low-n oligomers of tau protein promotes clearance of tau in cells via lysosomes

16. Suppressing Tau Aggregation and Toxicity by an Anti-Aggregant Tau Fragment

17. The Plasma Factor XIII Heterotetrameric Complex Structure: Unexpected Unequal Pairing within a Symmetric Complex

18. Disruption of Structural Disulfides of Coagulation FXIII-B Subunit; Functional Implications for a Rare Bleeding Disorder

19. Purification and Characterization of Low-n Tau Oligomers

20. Pathological missorting of endogenous MAPT/Tau in neurons caused by failure of protein degradation systems

21. Purification and Characterization of Low-n Tau Oligomers

22. C3G (RapGEF1), a regulator of actin dynamics promotes survival and myogenic differentiation of mouse mesenchymal cells

23. Extracellular low-n oligomers of tau cause selective synaptotoxicity without affecting cell viability

24. The release and trans-synaptic transmission of Tau via exosomes

25. Stages and Conformations of the Tau Repeat Domain during Aggregation and Its Effect on Neuronal Toxicity

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