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1. L-2-Hydroxyglutarate remodeling of the epigenome and epitranscriptome creates a metabolic vulnerability in kidney cancer models

2. Abstract B005: Metabolic liabilities in high L-2HG kidney cancer

4. Abstract 3705: L-2HG, oncometabolite-driven epigenetic and epitranscriptomic reprogramming creates metabolic vulnerability in renal cancer

5. PD17-08 EPIGENETIC AND EPITRANSCRIPTOMIC REPROGRAMMING IN RENAL CANCER BY ONCOMETABOLITE L-2HG CREATES METABOLIC VULNERABILITY

7. The TGF-β/HDAC7 axis suppresses TCA cycle metabolism in renal cancer

8. Enhancement of anti-inflammatory and immunomodulatory effects of adipose-derived human mesenchymal stem cells by making uniform spheroid on the new nano-patterned plates

10. Anemic copper-deficient rats, but not mice, display low hepcidin expression and high ferroportin levels

11. TGF-β signaling suppresses TCA cycle metabolism in renal cancer

12. PGC1α suppresses kidney cancer progression by inhibiting collagen-induced SNAIL expression

13. PRDM16 suppresses HIF-targeted gene expression in kidney cancer

14. 14-3-3 proteins protect AMPK-phosphorylated ten-eleven translocation-2 (TET2) from PP2A-mediated dephosphorylation

15. Teleological Role of L-2-Hydroxyglutarate Dehydrogenase in the Kidney

16. Abstract 5482: L-2HG/ L2HGDH axis as therapeutic target for kidney cancer

17. Abstract 4483: Functional implications ofPRDM16loss in kidney cancer

19. Anemic Copper-Deficient Rats, but Not Mice, Display Low Hepcidin Expression and High Ferroportin Levels1–3

21. Synergistic Inhibitory Effects of Hypoxia and Iron Deficiency on Hepatic Glucose Response in Mouse Liver.

29. ZIP14 and DMT1 in the liver, pancreas, and heart are differentially regulated by iron deficiency and overload: implications for tissue iron uptake in iron-related disorders.

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