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2. Ketolysis drives CD8+ T cell effector function through effects on histone acetylation

6. DNA methylation dynamics and dysregulation delineated by high-throughput profiling in the mouse

8. 13 C metabolite tracing reveals glutamine and acetate as critical in vivo fuels for CD8 T cells

11. 13C metabolite tracing reveals glutamine and acetate as critical in vivo fuels for CD8+T cells

12. The histone lysine demethylase KDM5C fine-tunes gene expression to regulate dendritic cell heterogeneity and function

13. LKB1 controls inflammatory potential through CRTC2-dependent epigenetic remodeling

14. Inhibition of the mitochondrial pyruvate carrier simultaneously mitigates hyperinflammation and hyperglycemia in COVID-19

16. Human alveolar macrophage metabolism is compromised during Mycobacterium tuberculosis infection

17. Evolutionary Landscape of SOX Genes to Inform Genotype-to-Phenotype Relationships

19. Ketolysis is a metabolic driver of CD8+ T cell effector function through histone acetylation

22. DNA Methylation Dynamics and Dysregulation Delineated by High-Throughput Profiling in the Mouse

23. ACLY and ACSS2 link nutrient-dependent chromatin accessibility to CD8 T cell effector responses

24. 13C metabolite tracing reveals glutamine and acetate as critical in vivo fuels for CD8 T cells.

25. The histone demethylase KDM5C controls female bone mass by promoting energy metabolism in osteoclasts.

26. Dietary Restriction Enhances CD8⁺ T Cell Ketolysis to Limit Exhaustion and Boost Anti-Tumor Immunity.

27. Glucose-dependent glycosphingolipid biosynthesis fuels CD8 + T cell function and tumor control.

28. NRF2-dependent regulation of the prostacyclin receptor PTGIR drives CD8 T cell exhaustion.

29. Inhibiting the MNK1/2-eIF4E axis impairs melanoma phenotype switching and potentiates antitumor immune responses.

30. 13 C metabolite tracing reveals glutamine and acetate as critical in vivo fuels for CD8 + T cells.

31. The histone demethylase KDM5C controls female bone mass by promoting energy metabolism in osteoclasts.

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