THE C3-ACTIVATOR SYSTEM: AN ALTERNATE PATHWAY OF COMPLEMENT ACTIVATION

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MEDIATION OF IMMUNOLOGICAL INJURY

THE C3-ACTIVATOR SYSTEM: AN ALTERNATE PATHWAY OF COMPLEMENT ACTIVATION

Otto Götze ¹ and Hans J. Müller-Eberhard ¹

¹ From the Department of Experimental Pathology, Scripps Clinic and Research Foundation, La Jolla, California 92037

Evidence has accumulated indicating the existence of a secondcomplement activation mechanism which is functionally analogousto C1, C2, and C4. The noncomplement protein C3PA, previouslyrecognized through its ability to form a complex enzyme witha protein from cobra venom, appears to be the precursor of theC4,2 analogue. It is a thermolabile ß-globulin with a molecularweight of 80,000. When serum is treated with naturally occurringplant or bacterial polysaccharides, the C3PA is cleaved intoat least two fragments, one having the electrophoretic mobilityof a $gamma$ -globulin and a molecular weight of 60,000, and the otherbeing an acidic peptide with a molecular weight of 20,000. Thelarger fragment has the ability to cleave C3 into C3a and C3band is therefore called C3 activator. It arises from the actionof an as yet unidentified serum enzyme upon the C3PA, whichis tentatively called C3PA convertase. In addition to endotoxins,yeast cell walls, inulin, and agar, aggregates of immunoglobulinswere found to be activating substances, including human IgA,guinea pig $gamma$ 1, and duck antibody. Serum depleted of C3PA hadreduced E. coli bactericidal and increased hemolytic activity.The relationship of the C3-activator system to experimentaland clinical observations has been discussed.

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