Abstract
Incubation of purified human plasma prekallikrein with sulfatides or dextran sulfate resulted in spontaneous activation of prekallikrein as judged by the appearance of amidolytic activity toward the chromogenic substrate H-D-Pro-Phe-Arg-p-nitroanilide. The time course of generation of amidolytic activity was sigmoidal with an apparent lag phase that was followed by a relatively rapid activation until finally a plateau was reached. Soybean trypsin inhibitor completely blocked prekallikrein activation whereas corn, lima bean, and ovomucoid trypsin inhibitors did not. The Ki of the reversible inhibitor benzamidine for autoactivation (240 microM) was identical to the Ki of benzamidine for kallikrein. Thus, spontaneous prekallikrein activation and kallikrein showed the same specificity for a number of serine protease inhibitors. This indicates that prekallikrein is activated by its own enzymatically active form, kallikrein. Immunoblotting analysis of the time course of activation showed that, concomitant with the appearance of amidolytic activity, prekallikrein was cleaved. However, prekallikrein was not quantitatively converted into two-chain kallikrein since other polypeptide products were visible on the gels. This accounts for the observation that in amidolytic assays not all prekallikrein present in the reaction mixture was measured as active kallikrein. Kinetic analysis showed that prekallikrein activation can be described by a second-order reaction mechanism in which prekallikrein is activated by kallikrein. The apparent second-order rate constant was 2.7 X 10(4) M-1 s-1 (pH 7.2, 50 microM sulfatides, ionic strength I = 0.06, at 37 degrees C). Autocatalytic prekallikrein activation was strongly dependent on the ionic strength, since there was a considerable decrease in the second-order rate constant of the reaction at high salt concentrations. In support of the autoactivation mechanism it was found that increasing the amount of kallikrein initially present in the reaction mixture resulted in a significant reduction of the lag period and a rapid completion of the reaction while the second-order rate constant was not influenced. Our data support a prekallikrein autoactivation mechanism in which surface-bound kallikrein activates surface-bound prekallikrein.
Highlights
From the $Department of Biochemistry, Universityof Limburg, 6200 MD Maastricht, The Netherlandsand Department of Immunology, Scripps Clinicand Research Foundation, La Jolla, California 92037
Incubation of purified human plasma prekallikrein Human plasma prekallikrein is the zymogen of aserine with sulfatides or dextran sulfate resulted in sponta- protease which circulates in the blood
Incubation of plasma neous activation of prekallikrein as judged by the ap- with negatively charged surfaces such as glass, kaolin, sulfapearance of amidolytic activity toward the chromo- tides, or dextran sulfate results in contacatctivation, a process genic substrate H-D-Pro-Phe-Arg-p-nitroanilideT.he during which the zymogen prekallikrein becomes activated to time course of generation of amidolytic activity was kallikrein through limited proteolysis
Summary
Guido Tans$$,J a n RosingS, Mauro Berrettini, BernhardLammle, and JohnH. Griffin. Prekallikrein was observed that under certain experimental conditions incubanot quantitatively converted into two-chain kallikreintion of purified prekallikrein with surfaces such as sulfatides since other polypeptide products were visible on the or dextran sulfate resulted in spontaneous activation of the gels. This accounts for the observationthat inamidol- zymogen. Kinetic analysis showed that prekallikrein activation can be described by a second-order reaction mechanism in which prekallikreinisactivated by kallikrein.The apparent second-order rate constant was2.7 X lo4M”. All other materials were of the highest grade commercially available
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