A requirement for specific cellular collaboration has been demonstrated for the induction of humoral antibody (1-3), cytotoxic T cells (4,5), and for those helper T cells able to help the induction of B cells (6). Leung and Ada (7) have recently shown that antigen-specific cells can significantly enhance the primary in vitro induction of delayed-type hypersensitivity (DTH)a to influenza virus. We independently developed an in vitro system in which the induction of significant DTH reactivity is dependent on the presence of antigen-specific helper T cells. We used this system to determine the antigen recognition requirements by which these helper T cells act in the induction of DTH precursor cells.A phenomenon referred to as carrier specificity in the elicitation of DTH has been reported in the literature (8, 9), i.e., animals sensitized to a hapten on a given carrier will respond with DTH reactivity only when challenged with the hapten on the same carrier as was used for sensitization. This phenomenon has been insufficiently characterized to ascertain whether it is simply quantitative, in that only a small amount of the DTH reactivity is directed against the hapten, or whether it reflects either a requirement for specific cellular collaboration in the elicitation of DTH and/or that the DTH effector cells are specific for neoantigenic determinants created by coupling the hapten to the carrier. In any case, the phenomenon does not bear on the cellular requirements for inducing DTH and is in this sense different from the classical carrier effects described for the induction of humoral responses.The mechanism by which antigen-specific cells cooperate in the induction of B and helper T cells is known to be most effective when the two specific classes of cells recognize determinants that are physically linked to one another (10,11). With the recent establishment of experimental systems that allow DTH to be induced in vitro (12, 13), it has become possible to determine the cellular requirements for the induction of DTH. The experiments described in this paper were designed to test whether (a) specific cellular collaboration was required for the induction of DTH and * Supported by a grant from the Medical Research Council of Canada to the MRC group on immunoregulation, and a studentship and research allowance from the Alberta Heritage Foundation for Medical Research awarded to M. J. Tucker.1 Abbreviations used in this paper: BRBC, burro erythrocytes; CRBC, chicken erythrocytes; DTH, delayedtype hypersensitivity; FCS, fetal calf serum; FGG, fowl gamma globulin; FGG-BRBC, fowl gamma globulin physically coupled to burro erythrocytes; FGG-MRBC, fowl gamma globulin physically coupled to mouse erythrocytes; i.v., intravenous; MRBC, mouse erythrocytes; RBC, erytbrocytes; s.c., subcutaneous; Thy-1, thymus-derived cell marker.J. Exo. MED.
