ACTIVATION OF HAGEMAN FACTOR IN SOLID AND FLUID PHASES: A CRITICAL ROLE OF KALLIKREIN

doi:10.1084/jem.138.6.1564

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ARTICLE

ACTIVATION OF HAGEMAN FACTOR IN SOLID AND FLUID PHASES : A CRITICAL ROLE OF KALLIKREIN

C. G. Cochrane ¹, S. D. Revak ¹, and K. D. Wuepper ¹

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

The activation of Hageman factor in solid and fluid phase hasbeen analyzed. Activation of highly purified Hageman factoroccurred after it interacted with and became bound to a negativelycharged surface. Activation was observed in the absence of enzymesthat are inhibitable with diisopropylfluorophosphate, phenylmethyl sulfonyl fluoride and $epsi$ -amino-n-caproic acid. The bindingof [¹²⁵I]Hageman factor to the negatively chargedsurface was markedly inhibited by plasma or purified plasmaproteins.

Activation of Hageman factor in solution (fluid phase)was obtained with kallikrein, plasmin, and Factor XI (plasmathromboplastin antecedent). Kallikrein was greater than 10 timesmore active in its ability to activate Hageman factor than plasminand Factor XI. The data offer a plausible explanation for thefinding that highly purified kallikrein promotes clotting ofnormal plasma. In addition, the combined results of this andpreviously reported data from this laboratory indicate thatthe reciprocal activation of Hageman factor by kallikrein influid phase is essential for normal rate of activation of theintrinsic-clotting, kinin-forming, and fibrinolytic systems.

Activationof Hageman factor was associated with three different structuralchanges in the molecule: (a) Purified Hageman factor, activatedon negatively charged surfaces retained its native mol wt of80–90,000. Presumably a conformational change accompaniedactivation. (b) In fluid phase, activation with kallikrein andplasmin did not result in cleavage of large fragments of rabbitHageman factor, although the activation required hydrolyticcapacity of the enzymes. (c) Activation of human Hageman factorwith kallikrein or plasmin was associated with cleavage of themolecule to 52,000, 40,000, and 28,000 mol wt fragments. Activationof rabbit Hageman factor with trypsin resulted in cleavage ofthe molecule into three fragments, each of 30,000 mol wt asnoted previously. This major cleavage occurred simultaneouslywith activation.

Submitted on July 23, 1973

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