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1. RUNX2 regulates leukemic cell metabolism and chemotaxis in high-risk T cell acute lymphoblastic leukemia

7. Respiratory burst oxidase activation can be dissociated from phosphatidylinositol bisphosphate degradation in a cell-free system from human neutrophils

8. Nitric oxide/cGMP pathway signaling actively down-regulates α4β1-integrin affinity: an unexpected mechanism for inducing cell de-adhesion

9. Galphas-coupled receptor signaling actively down-regulates α4β1-integrin affinity: A possible mechanism for cell de-adhesion

10. Best practices for managing and disseminating resources and outreach and evaluating the impact of the IDG Consortium.

11. A Flow Cytometry-Based High-Throughput Technique for Screening Integrin-Inhibitory Drugs.

12. The FDA-approved compound, pramipexole and the clinical-stage investigational drug, dexpramipexole, reverse chronic allodynia from sciatic nerve damage in mice, and alter IL-1β and IL-10 expression from immune cell culture.

13. A phenotypic screen for compounds that reverse cAMP-mediated suppression of T cell functions.

14. RUNX2 regulates leukemic cell metabolism and chemotaxis in high-risk T cell acute lymphoblastic leukemia.

15. Inhibition of the HEG1-KRIT1 interaction increases KLF4 and KLF2 expression in endothelial cells.

16. Drug repurposing for targeting cyclic nucleotide transporters in acute leukemias - A missed opportunity.

17. Virtual and In Vitro Antiviral Screening Revive Therapeutic Drugs for COVID-19.

18. Pyrazole-Based Lactate Dehydrogenase Inhibitors with Optimized Cell Activity and Pharmacokinetic Properties.

19. A Novel Flow Cytometric Assay to Identify Inhibitors of RBPJ-DNA Interactions.

20. Dynamic Imaging of LDH Inhibition in Tumors Reveals Rapid In Vivo Metabolic Rewiring and Vulnerability to Combination Therapy.

21. A Selective Ligand for Estrogen Receptor Proteins Discriminates Rapid and Genomic Signaling.

22. Autophagy, Inflammation, and Metabolism (AIM) Center in its second year.

23. Clioquinol: To harm or heal.

24. Far away from the lamppost.

25. High-Throughput Screening Approach for Identifying Compounds That Inhibit Nonhomologous End Joining.

26. A High-Throughput Flow Cytometry Screen Identifies Molecules That Inhibit Hantavirus Cell Entry.

27. High-Throughput Flow Cytometry Identifies Small-Molecule Inhibitors for Drug Repurposing in T-ALL.

28. High-Throughput Flow Cytometry Drug Combination Discovery with Novel Synergy Analysis Software, SynScreen.

29. Evaluating integrin activation with time-resolved flow cytometry.

30. Activation of Rho Family GTPases by Small Molecules.

31. Unexplored therapeutic opportunities in the human genome.

33. Functional and clinical relevance of VLA-4 (CD49d/CD29) in ibrutinib-treated chronic lymphocytic leukemia.

34. Autophagy, Inflammation, and Metabolism (AIM) Center of Biomedical Research Excellence: supporting the next generation of autophagy researchers and fostering international collaborations.

35. High-Throughput Flow Cytometry Screening of Multidrug Efflux Systems.

36. TIN-X: target importance and novelty explorer.

37. Pharos: Collating protein information to shed light on the druggable genome.

38. Novel ABCG2 Antagonists Reverse Topotecan-Mediated Chemotherapeutic Resistance in Ovarian Carcinoma Xenografts.

39. Relationship of light scatter change and Cdc42-regulated actin status.

40. Inhibition of Dihydroorotate Dehydrogenase Overcomes Differentiation Blockade in Acute Myeloid Leukemia.

41. Targeting efflux pumps to overcome antifungal drug resistance.

42. Cyclic AMP efflux inhibitors as potential therapeutic agents for leukemia.

43. Badapple: promiscuity patterns from noisy evidence.

44. Sulindac sulfide selectively increases sensitivity of ABCC1 expressing tumor cells to doxorubicin and glutathione depletion.

45. A High-Throughput Flow Cytometry Assay for Identification of Inhibitors of 3',5'-Cyclic Adenosine Monophosphate Efflux.

46. Discovery of Small-Molecule Nonfluorescent Inhibitors of Fluorogen-Fluorogen Activating Protein Binding Pair.

47. A Novel Pharmacologic Activity of Ketorolac for Therapeutic Benefit in Ovarian Cancer Patients.

48. Novel Activities of Select NSAID R-Enantiomers against Rac1 and Cdc42 GTPases.

49. R-Ketorolac Targets Cdc42 and Rac1 and Alters Ovarian Cancer Cell Behaviors Critical for Invasion and Metastasis.

50. A Pan-GTPase Inhibitor as a Molecular Probe.

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