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1. Genetic Deletion of FXR1 Reduces Intimal Hyperplasia and Induces Senescence in Vascular Smooth Muscle Cells.

2. Regulation of Stress Granule Formation by Inflammation, Vascular Injury, and Atherosclerosis.

3. RNA stability protein ILF3 mediates cytokine-induced angiogenesis.

4. FXR1 Is an IL-19-Responsive RNA-Binding Protein that Destabilizes Pro-inflammatory Transcripts in Vascular Smooth Muscle Cells.

5. Genetic Deletion of IL-19 (Interleukin-19) Exacerbates Atherogenesis in Il19 -/- × Ldlr -/- Double Knockout Mice by Dysregulation of mRNA Stability Protein HuR (Human Antigen R).

6. Induction of MiR133a expression by IL-19 targets LDLRAP1 and reduces oxLDL uptake in VSMC.

7. Interleukin-19 induces angiogenesis in the absence of hypoxia by direct and indirect immune mechanisms.

8. Interleukin-19 increases angiogenesis in ischemic hind limbs by direct effects on both endothelial cells and macrophage polarization.

9. IL-19 reduces ligation-mediated neointimal hyperplasia by reducing vascular smooth muscle cell activation.

10. Attenuation of experimental atherosclerosis by interleukin-19.

11. Interleukin-19 (IL-19) induces heme oxygenase-1 (HO-1) expression and decreases reactive oxygen species in human vascular smooth muscle cells.

12. Increased atherosclerosis and vascular smooth muscle cell activation in AIF-1 transgenic mice fed a high-fat diet.

13. The anti-inflammatory cytokine interleukin 19 is expressed by and angiogenic for human endothelial cells.

14. AIF-1 expression regulates endothelial cell activation, signal transduction, and vasculogenesis.

15. Inhibition of allograft inflammatory factor-1 expression reduces development of neointimal hyperplasia and p38 kinase activity.

16. Small airway mucous metaplasia and inflammation in chronic obstructive pulmonary disease.

17. Expression and suppressive effects of interleukin-19 on vascular smooth muscle cell pathophysiology and development of intimal hyperplasia.

18. Increased smooth muscle cell activation and neointima formation in response to injury in AIF-1 transgenic mice.

19. Inhibition of AIF-1 expression by constitutive siRNA expression reduces macrophage migration, proliferation, and signal transduction initiated by atherogenic stimuli.

20. Expression of allograft inflammatory factor-1 in T lymphocytes: a role in T-lymphocyte activation and proliferative arteriopathies.

21. Expression of granulocyte colony-stimulating factor is induced in injured rat carotid arteries and mediates vascular smooth muscle cell migration.

22. Early growth responsive gene (Egr)-1 expression correlates with cardiac allograft rejection.

23. AIF-1 expression modulates proliferation of human vascular smooth muscle cells by autocrine expression of G-CSF.

24. AIF-1 is an actin-polymerizing and Rac1-activating protein that promotes vascular smooth muscle cell migration.

25. Quantitative assessment of cell adhesion molecule gene expression in endomyocardial biopsy specimens from cardiac transplant recipients using competitive polymerase chain reaction.

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