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1. Cerebrospinal fluid and plasma biomarkers in individuals at risk for genetic prion disease

2. Modulation of prion protein expression through cryptic splice site manipulation.

3. Fluid Biomarkers in Individuals at Risk for Genetic Prion Disease up to Disease Conversion.

4. Brainwide silencing of prion protein by AAV-mediated delivery of an engineered compact epigenetic editor.

5. Evidence that minocycline treatment confounds the interpretation of neurofilament as a biomarker.

6. Modulation of prion protein expression through cryptic splice site manipulation.

7. Biomarker changes preceding symptom onset in genetic prion disease.

8. A single-cell map of antisense oligonucleotide activity in the brain.

10. Therapeutic Trial of anle138b in Mouse Models of Genetic Prion Disease.

11. Disease stages and therapeutic hypotheses in two decades of neurodegenerative disease clinical trials.

12. Genetic counseling for prion disease: Updates and best practices.

13. Analysis of non-human primate models for evaluating prion disease therapeutic efficacy.

14. Regional variability and genotypic and pharmacodynamic effects on PrP concentration in the CNS.

15. Novel quaternary structures of the human prion protein globular domain.

17. Prion protein lowering is a disease-modifying therapy across prion disease stages, strains and endpoints.

18. Multimodal small-molecule screening for human prion protein binders.

19. Cerebrospinal fluid and plasma biomarkers in individuals at risk for genetic prion disease.

20. Towards a treatment for genetic prion disease: trials and biomarkers.

21. The Patient-Scientist's Mandate.

22. Characterization of the Prion Protein Binding Properties of Antisense Oligonucleotides.

23. Domain-specific Quantification of Prion Protein in Cerebrospinal Fluid by Targeted Mass Spectrometry.

24. Antisense oligonucleotides extend survival of prion-infected mice.

25. Age at onset in genetic prion disease and the design of preventive clinical trials.

26. Prion protein quantification in human cerebrospinal fluid as a tool for prion disease drug development.

27. Quantifying prion disease penetrance using large population control cohorts.

28. Htt CAG repeat expansion confers pleiotropic gains of mutant huntingtin function in chromatin regulation.

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