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1. Data characterizing the ZMIZ1 molecular phenotype of multiple sclerosis

2. The CYP27B1 variant associated with an increased risk of autoimmune disease is underexpressed in tolerizing dendritic cells

3. A Transcription Factor Map as Revealed by a Genome-Wide Gene Expression Analysis of Whole-Blood mRNA Transcriptome in Multiple Sclerosis

4. Response to interferon-beta treatment in multiple sclerosis patients: a genome-wide association study

5. Expression of CYP24A1 and other multiple sclerosis risk genes in peripheral blood indicates response to vitamin D in homeostatic and inflammatory conditions.

6. Evidence from genome wide association studies implicates reduced control of Epstein-Barr virus infection in multiple sclerosis susceptibility.

7. Association of Regulatory T-Cell Expansion With Progression of Amyotrophic Lateral Sclerosis: A Study of Humans and a Transgenic Mouse Model.

8. Response to interferon-beta treatment in multiple sclerosis patients: a genome-wide association study.

9. The autoimmune risk gene ZMIZ1 is a vitamin D responsive marker of a molecular phenotype of multiple sclerosis.

10. Data characterizing the ZMIZ1 molecular phenotype of multiple sclerosis.

11. Differences in common heritable blood immune cell populations may underlie MS susceptibility and progression.

12. The low EOMES/TBX21 molecular phenotype in multiple sclerosis reflects CD56+ cell dysregulation and is affected by immunomodulatory therapies.

13. Ribosomal protein S6 mRNA is a biomarker upregulated in multiple sclerosis, downregulated by interferon treatment, and affected by season.

14. The CYP27B1 variant associated with an increased risk of autoimmune disease is underexpressed in tolerizing dendritic cells.

15. The autoimmune disease-associated transcription factors EOMES and TBX21 are dysregulated in multiple sclerosis and define a molecular subtype of disease.

16. IL7Rα expression and upregulation by IFNβ in dendritic cell subsets is haplotype-dependent.

17. A transcription factor map as revealed by a genome-wide gene expression analysis of whole-blood mRNA transcriptome in multiple sclerosis.

18. The multiple sclerosis whole blood mRNA transcriptome and genetic associations indicate dysregulation of specific T cell pathways in pathogenesis.

19. Novel approaches to detect serum biomarkers for clinical response to interferon-beta treatment in multiple sclerosis.

20. Functionally significant differences in expression of disease-associated IL-7 receptor alpha haplotypes in CD4 T cells and dendritic cells.

21. Parameters governing invasive disease propensity of non-M1 serotype group A streptococci.

22. BAFF is a biological response marker to IFN-beta treatment in multiple sclerosis.

23. Allelic variants of streptokinase from Streptococcus pyogenes display functional differences in plasminogen activation.

24. CD127 immunophenotyping suggests altered CD4+ T cell regulation in primary progressive multiple sclerosis.

25. Haplotypes of the interleukin 7 receptor alpha gene are correlated with altered expression in whole blood cells in multiple sclerosis.

26. Trigger for group A streptococcal M1T1 invasive disease.

27. Plasminogen binding by group A streptococcal isolates from a region of hyperendemicity for streptococcal skin infection and a high incidence of invasive infection.

29. The human ventilatory response to stimulation by transient hypoxia.

30. The optical isomers of metaraminol. Synthesis and biological activity.

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