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1. Galectin-9 – ligand axis: an emerging therapeutic target for multiple myeloma

2. The role of galectins in mediating the adhesion of circulating cells to vascular endothelium

3. Galectins can serve as biomarkers in COVID-19: A comprehensive systematic review and meta-analysis

5. Loss of GCNT2/I-branched glycans enhances melanoma growth and survival

6. Data from Inhibition of Melanoma Cell–Intrinsic Tim-3 Stimulates MAPK-Dependent Tumorigenesis

7. Supplementary Data from Inhibition of Melanoma Cell–Intrinsic Tim-3 Stimulates MAPK-Dependent Tumorigenesis

8. Supplementary Figure 5 from Definition of Molecular Determinants of Prostate Cancer Cell Bone Extravasation

10. Supplementary Figure 4 from Definition of Molecular Determinants of Prostate Cancer Cell Bone Extravasation

13. Supplementary Figure 2 from Definition of Molecular Determinants of Prostate Cancer Cell Bone Extravasation

14. Supplementary Movie 2 from Definition of Molecular Determinants of Prostate Cancer Cell Bone Extravasation

15. Supplementary Figure 3 from Definition of Molecular Determinants of Prostate Cancer Cell Bone Extravasation

16. Human B Cell Differentiation Is Characterized by Progressive Remodeling of O-Linked Glycans

17. Galectin-Glycan Interactions as Regulators of B Cell Immunity

20. Abstract 3602: The metastasis-suppressive function of intracellular galectin-3 in melanoma

21. Hypoxia Controls the Glycome Signature and Galectin-8–Ligand Axis to Promote Protumorigenic Properties of Metastatic Melanoma

22. Analysis of Galectin-Binding Receptors on B Cells

23. Novel Methods and Pathways in Cancer Glycobiology Research

24. Deep Learning to Discover Cancer Glycome Genes Signifying the Origins of Cancer

25. Galectin-9 bridges human B cells to vascular endothelium while programming regulatory pathways

26. Galectin-9 suppresses B cell receptor signaling and is regulated by I-branching of N-glycans

27. Cancer immunotherapy needs to learn how to stick to its guns

29. Glycan characterization of pregnancy-specific glycoprotein 1 and its identification as a novel Galectin-1 ligand

30. I-branched carbohydrates as emerging effectors of malignant progression

31. Abstract 2609: Hypoxia-mediated downregulation of GCNT2/I-antigen in metastatic melanoma accelerates disease progression and mortality

32. Galectin-Binding O-Glycosylations as Regulators of Malignancy

33. Human fucosyltransferase 6 enables prostate cancer metastasis to bone

34. Definition of Molecular Determinants of Prostate Cancer Cell Bone Extravasation

35. Galectins and their ligands: negative regulators of anti-tumor immunity

36. Galectin-1 inhibits the viability, proliferation, and Th1 cytokine production of nonmalignant T cells in patients with leukemic cutaneous T-cell lymphoma

37. Galectin-1 Triggers an Immunoregulatory Signature in Th Cells Functionally Defined by IL-10 Expression

38. Peracetylated 4-Fluoro-glucosamine Reduces the Content and Repertoire of N- and O-Glycans without Direct Incorporation

40. Skin-Homing Receptors on Effector Leukocytes Are Differentially Sensitive to Glyco-Metabolic Antagonism in Allergic Contact Dermatitis

41. Targeting selectins and selectin ligands in inflammation and cancer

43. Direct Real-Time Observation of E- and P-Selectin-Mediated Rolling on Cutaneous Lymphocyte-Associated Antigen Immobilized on Western Blots

44. Melanoma Cell Galectin-1 Ligands Functionally Correlate with Malignant Potential

45. Using a chimera to study the role of Galectin‐1 in immunological responses and tumor progression (LB91)

46. Cd44 Is a Major E-Selectin Ligand on Human Hematopoietic Progenitor Cells

47. A hematopoietic cell L-selectin ligand that is distinct from PSGL-1 and displays N-glycan–dependent binding activity

48. Anti-Angiogenic Activity of Selected Receptor Tyrosine Kinase Inhibitors, PD166285 and PD173074: Implications for Combination Treatment with Photodynamic Therapy

49. Cell SurfaceN-Acetylneuraminic Acid α2,3-Galactoside-Dependent Intercellular Adhesion of Human Colon Cancer Cells

50. Galectins and Disease Implications for Targeted Therapeutics

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