COMPLEMENT-DEPENDENT B-CELL ACTIVATION BY COBRA VENOM FACTOR AND OTHER MITOGENS?

doi:10.1084/jem.139.2.337

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ARTICLE

COMPLEMENT-DEPENDENT B-CELL ACTIVATION BY COBRA VENOM FACTOR AND OTHER MITOGENS?

Peter Dukor ¹, Gebhard Schumann ¹, Roland H. Gisler ¹, Manfred Dierich ¹, Wolfgang König ¹, Ulrich Hadding ¹, and Dieter Bitter-Suermann ¹

¹ From the Research Department, Pharmaceuticals Division, CIBA-GEIGY Limited, CH-4002 Basle, Switzerland and the Institut für Medizinische Mikrobiologie der Johannes-Gutenberg-Universität, D-65 Mainz, Germany

It has been proposed that two distinct signals are requiredfor the triggering of the precursors of antibody-forming bonemarrow-derived cells (B cells): (a) the binding of antigen orof a mitogen to the corresponding receptor sites on B-cell membranesand (b) the interaction of activated C3 with the C3 receptorof B lymphocytes. There is growing evidence that B-cell mitogensand T (thymus-derived cell)-independent antigens are capableof activating the alternate pathway of the complement system(bypass). Therefore, the effect of another potent bypass inducerwas investigated with regard to B-cell activation and the roleof C3. Purified, pyrogen-free cobra venom factor was mitogenicfor both T and B lymphocytes (cortisone-resistant mouse thymuscells and lymph node lymphocytes from congenitally athymic mice).Venom factor could substitute for T cells by restoring the potentialof antibody formation to sheep red blood cells in mouse B-cellcultures supplemented with macrophages or 2-mercaptoethanol.Venom factor may be capable of conferring activated C3 to theC3 receptor of B lymphocytes: preincubation of lymphoid cellswith homologous serum or plasma, 10 mM EDTA, and sepharose-coupledvenom factor converted with serum to an enzyme active againstC3, inhibited their capacity to subsequently form rosettes withsheep erythrocytes sensitized with amboceptor and C5-deficientmouse complement. In the absence of EDTA, preincubation of freshlyprepared B-cell suspensions with C3-sufficient homologous serumalso blocked their subsequent interaction with complement-sensitizederythrocytes and at the same time rendered them reactive toan otherwise T-cell-specific mitogen. Moreover, mitogen inducedB-cell proliferation in lymph node (but not in spleen) cellcultures, appeared to depend on the availability of exogenousC3: zymosan-absorbed fetal bovine serum (only 8.3% site-formingunits remaining) supported T-cell activation by phytohemagglutinin,concanavalin A, and venom factor, but failed to sustain B-cellstimulation by pokeweed mitogen, lipopolysaccharide, and venomfactor. T-cell-dependent antibody formation in composite culturescontaining T cells or T-cell-substituting B-cell mitogens, Bcells, and macrophages, always required the presence of C3-sufficientserum.

Submitted on August 31, 1973

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