CELL INTERACTIONS IN THE IMMUNE RESPONSE IN VITRO: V. SPECIFIC COLLABORATION VIA COMPLEXES OF ANTIGEN AND THYMUS-DERIVED CELL IMMUNOGLOBULIN

doi:10.1084/jem.136.4.737

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ARTICLE

CELL INTERACTIONS IN THE IMMUNE RESPONSE IN VITRO : V. SPECIFIC COLLABORATION VIA COMPLEXES OF ANTIGEN AND THYMUS-DERIVED CELL IMMUNOGLOBULIN

Marc Feldmann ¹

¹ From The Walter and Eliza Hall Institute of Medical Research, Melbourne, Victoria 3050, Australia

The mechanism of interaction of T and B lymphocytes was investigatedin an in vitro hapten carrier system using culture chamberswith two compartments separated by a cell impermeable nucleoporemembrane. Because specific cell interaction occurred efficientlyacross this membrane, contact of T and B lymphocytes was notessential for cooperation which must have been mediated by asubcellular component or "factor." By using different lymphoidcell populations in the lower culture chamber and activatedthymus cells in the upper chamber (with antigen present in both),it was found that the antigen-specific mediator acted indirectlyon B cells, through the agency of macrophages. Macrophages whichhad been cultured in the presence of activated T cells and antigenacquired the capacity to specifically induce antibody responsesin B cell-containing lymphoid populations. Trypsinization ofthese macrophages inhibited their capacity to induce immuneresponses, indicating that the mediator of cell cooperationis membrane bound. By using antisera to both the haptenic andcarrier determinants of the antigen as blocking reagents, itwas demonstrated that the whole antigen molecule was presenton the surface of macrophages which had been exposed to activatedT cells and antigen. Because specifically activated T cellswere essential a component of the antigen-specific mediatormust be derived from these cells. By using anti-immunoglobulinsera as inhibitors of the binding of the mediator to macrophages,the T cell component was indeed found to contain both $kappa$ - andµ-chains and was thus presumably a T cell-derived immunoglobulin.

Itwas proposed that cell cooperation is mediated by complexesof T cell IgM and antigen, bound to the surface of macrophage-likecells, forming a lattice of appropriately spaced antigenic determinants.B cells become immunized by interacting with this surface. Withthis mechanism of cell cooperation, the actual pattern of antigen-Bcell receptor interactions in immunization would be the samewith both thymus-dependent and independent antigens. An essentialfeature of the proposed mechanism of cell cooperation is thatmacrophage-B cell interaction must occur at an early stage ofthe antibody response, a concept which is supported by manylines of evidence. Furthermore this mechanism of cell interactioncan be elaborated to explain certain phenomena such as the highlyimmunogenic macrophage-bound antigen, antigenic competition,the distinction between immunity and tolerance in B lymphocytes,and the possible mediation of tolerance by T lymphocytes.

Submitted on April 24, 1972

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