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1. Loss of Anti-Tumor Efficacy by Polyamine Blocking Therapy in GCN2 Null Mice

2. Influence of apolipoprotein A-I and apolipoprotein A-II availability on nascent HDL heterogeneity

3. Structural and functional consequences of the Milano mutation (R173C) in human apolipoprotein A-I

4. The role of reverse cholesterol transport in animals and humans and relationship to atherosclerosis

5. Immunomodulatory role of thrombin in cancer progression

8. Harnessing the polyamine transport system to treat BRAF inhibitor-resistant melanoma

9. Polyamine Blocking Therapy Decreases Survival of Tumor-Infiltrating Immunosuppressive Myeloid Cells and Enhances the Antitumor Efficacy of PD-1 Blockade

10. A novel polyamine blockade therapy activates an anti-tumor immune response

11. Polyamine-stimulation of arsenic-transformed keratinocytes

12. Thrombin inhibition and cisplatin block tumor progression in ovarian cancer by alleviating the immunosuppressive microenvironment

13. Thrombin inhibition and cyclophosphamide synergistically block tumor progression and metastasis

14. Influence of Apolipoprotein A-I Domain Structure on Macrophage Reverse Cholesterol Transport in Mice

15. Structural and functional consequences of the Milano mutation (R173C) in human apolipoprotein A-I

16. Overexpression of Human 15( S )-Lipoxygenase-1 in RAW Macrophages Leads to Increased Cholesterol Mobilization and Reverse Cholesterol Transport

17. Molecular mechanisms responsible for the differential effects of apoE3 and apoE4 on plasma lipoprotein-cholesterol levels

18. Hepatic sortilin regulates both apolipoprotein B secretion and LDL catabolism

19. Macrophage reverse cholesterol transport in mice expressing ApoA-I Milano

20. Wild-type ApoA-I and the Milano variant have similar abilities to stimulate cellular lipid mobilization and efflux

21. Abstract 392: Synergistic anti-tumor effects of dabigatran etexilate and cyclophosphamide co-treatment are associated with decreased circulating tissue factor positive microparticles

22. Intermolecular contact between globular N-terminal fold and C-terminal domain of ApoA-I stabilizes its lipid-bound conformation: studies employing chemical cross-linking and mass spectrometry

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