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1. Cutaneous immunization rapidly activates liver invariant Valpha14 NKT cells stimulating B-1 B cells to initiate T cell recruitment for elicitation of contact sensitivity.

2. B cell-dependent T cell responses: IgM antibodies are required to elicit contact sensitivity.

3. Required early complement activation in contact sensitivity with generation of local C5-dependent chemotactic activity, and late T cell interferon gamma: a possible initiating role of B cells.

4. Gamma delta T cells from tolerized alpha beta T cell receptor (TCR)-deficient mice inhibit contact sensitivity-effector T cells in vivo, and their interferon-gamma production in vitro.

5. An early component of delayed-type hypersensitivity mediated by T cells and mast cells.

6. Role of antigen-presenting cells in the development and persistence of contact hypersensitivity.

7. Specialized antigen-presenting cells. Splenic dendritic cells and peritoneal-exudate cells induced by mycobacteria activate effector T cells that are resistant to suppression.

8. T cells produce an antigen-binding factor with in vivo activity analogous to IgE antibody.

9. Augmentation of delayed-type hypersensitivity by doses of cyclophosphamide which do not affect antibody responses.

10. Nylon adherent antigen-specific rosette-forming T cells.

11. Suppression of T cell-mediated cutaneous basophil hypersensitivity by serum from guinea pigs immunized with mycobacterial adjuvant.

12. Requirement for vasoactive amines for production of delayed-type hypersensitvity skin reactions.

13. Serotonin storage pools in basophil leukemia and mast cells: characterization of two types of serotonin binding protein and radioautographic analysis of the intracellular distribution of [3H]serotonin.

14. T cell-dependent mast cell degranulation and release of serotonin in murine delayed-type hypersensitivity.

15. Cutaneous basophil hypersensitivity in contact-sensitized guinea pigs. I. Transfer with immune serum.

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