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1. Molecular Characteristics, Functional Definitions, and Regulatory Mechanisms for Cross-Presentation Mediated by the Major Histocompatibility Complex: A Comprehensive Review.

2. Cross-presentation of Exogenous Antigens.

3. A simulation of the random and directed motion of dendritic cells in chemokine fields.

4. Analysis of pattern formation and phase separation in the immunological synapse.

5. In vitro uptake of oligomannose-coated liposomes leads to differentiation of inflammatory monocytes into mature antigen-presenting cells that can activate T cells.

6. Regulatory T Cells in Human Ovarian Cancer.

7. Generation of antigen-specific cytotoxic T lymphocytes using a leukemic plasmacytoid dendritic cell line as antigen presenting cells

8. Thymic Selection of T Cells as Diffusion with Intermittent Traps.

9. Advantage of having regulatory T cells requires localized suppression of immune reactions

10. B-cells get the T-cells but antibodies get the worms

11. Human CD1 dimeric proteins as indispensable tools for research on CD1-binding lipids and CD1-restricted T cells

12. The role of low avidity T cells in the protection against type 1 diabetes: A modeling investigation

13. A Population Dynamics Analysis of the Interaction between Adaptive Regulatory T Cells and Antigen Presenting Cells.

14. Influence of High-Fat Feeding on Both Naive and Antigen-Experienced T-Cell Immune Response in DO10.11 Mice.

15. Normal Structure, Function, and Histology of Lymph Nodes.

16. Plasmacytoid dendritic cells and the regulation of immunoglobulin heavy chain class switching.

17. Non-responsiveness to hepatitis B surface antigen vaccines is not caused by defective antigen presentation or a lack of B7 co-stimulation.

18. Clinical application of dendritic cells in cancer vaccination therapy.

19. <atl>Effect of liposomal antigens on the priming and activation of the immune system by dendritic cells

20. The Role of Nanovaccine in Cross-Presentation of Antigen-Presenting Cells for the Activation of CD8+ T Cell Responses.

21. Contact time periods in immunological synapse.