CELLULAR INTERACTIONS IN THE PROLIFERATIVE RESPONSE OF HUMAN T AND B LYMPHOCYTES TO PHYTOMITOGENS AND ALLOGENEIC LYMPHOCYTES

doi:10.1084/jem.139.6.1553

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CELLULAR INTERACTIONS IN THE PROLIFERATIVE RESPONSE OF HUMAN T AND B LYMPHOCYTES TO PHYTOMITOGENS AND ALLOGENEIC LYMPHOCYTES

Hans-Peter Lohrmann ¹, Ligita Novikovs ¹, and Robert G. Graw Jr. ¹

¹ From the Experimental Hematology Section, Pediatric Oncology Branch, National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20014

In vitro studies were performed to determine the proliferativeresponsiveness of human peripheral blood thymus-dependent (T)and thymus-independent (B) lymphocytes to phytomitogens andallogeneic lymphocytes. Recombination of T and B cells, withselective inhibition of proliferation of one of the two populations,was used to identify cellular interactions which may contributeto cell proliferation. The distinctive feature of human T lymphocytesto form rosettes with unsensitized sheep erythrocytes was utilizedto separate human peripheral blood lymphocytes into highly purifiedresetting (T) and non-rosetting (B) cells. The proliferativeresponse of these separated lymphocyte subpopulations to variousstimulants was assessed from the uptake of tritiated thymidineinto DNA.

Phytohemagglutinin, concanavalin A, pokeweed mitogen,and allogeneic lymphocytes stimulated separated T cells, whereasno proliferation was observed with the T-cell-depleted B-cellpopulation. This suggests that it is the human T cell whichis activated directly by these stimulants. In the presence ofT cells (proliferating or nonproliferating), B cells were capableof proliferation following stimulation with phytomitogens, butnot in response to histocompatibility antigens. Thus, T-cell-mediatedB-cell proliferation contributes to the overall lymphocyte responsein phytomitogen-stimulated T + B cell mixtures, but not in humanmixed leukocyte cultures. T-cell activation by allogeneic cellsrequired the presence of monocytes; in contrast, the three testedphytomitogens stimulated T cells in the absence of monocytes.This indicates that direct interaction of mitogens with lymphocytemembrane receptors is sufficient to trigger T cells into proliferativeresponse. However, monocytes considerably enhanced the proliferativeresponse of T cells in a dose-dependent fashion; this monocyte-dependentmechanism of T-cell activation was predominant at lower concentrationsof phytomitogens, and contributed relatively less at highermitogen doses. Both, the direct, monocyte-independent, and theindirect, monocyte-dependent T-lymphocyte activation contributeto the total in vitro response of lymphocyte preparations tophytomitogens.

Submitted on February 26, 1974

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