Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: EC:3.4.21.5 (
thrombin
)
33,306
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Factors affecting the coagulant activity of two different prothrombin complex concentrates have been investigated using a sensitive in vitro assay developed in this laboratory. One concentrate contained substantial amounts of potentially thrombogenic material, while the other, which was deliberately fortified with
antithrombin III
and heparin during production, was judged to be relatively nonthrombogenic. The coagulant activity of the thrombogenic concentrate has been partially identified and was due largely to the presence of coagulation factos IXa and Xa. Neither concentrate contained detectable
thrombin
. However, after incubation with calcium or various polyamines, large amounts of additional coagulant material, including
thrombin
, appeared. Heparin and
antithrombin III
not only neutralized the thrombogenic materials present in the thrombogenic concentrate, but also inhibited the de novo generation of coagulant enzymes during incubation with calcium. The implication of these studies on the preparation of prothrombin complex concentrates and on host susceptibility to thrombosis during the clinical use of these concentrates is discussed.
...
PMID:Prothrombin complex concentrates: potentially thrombogenic materials and clues to the mechanism of thrombosis in vivo. 1 45
By devising and applying quantitative methods for the assay of
thrombin
and autoprothrombin C and by developing techniques for their purification, it was possible to obtain information about the function and properties of antithrombin. The inhibitor is a protein for which the initial purification steps consist of removing fibrinogen from plasma by heating to 56 degrees for 3 min, removing prothrombin complex by absorption on barium carbonate, absorbing the antithrombin on aluminum hydroxide, and eluting with phosphate buffer. Antithrombin is limited in its capacity to neutralize
thrombin
activity, and, under some conditions, the rate of inhibition was accelerated, but equivocal results were involved. Heparin cofactor was found to be essential for retarding the formation of
thrombin
, and, by inference, it is essential for retarding the formation of autoprothrombin C. Heparin cofactor and
antithrombin III
are the same. Thrombin absorbs on fibrin, and this has been referred to as the "antithrombin I effect." Interference with the
thrombin
-fibrinogen reaction by mixtures of
antithrombin III
and heparin is called the "antithrombin II henomenon." The acceleration of
thrombin
inactivation at the time
thrombin
forms is called the "antithrombin IV effect." It was discovered that
antithrombin III
neutralizes
thrombin
, as well as autoprothrombin C. The inhibitor and the enzyme form a mutual depletion system. To assay for
antithrombin III
, a standard quantity of
thrombin
(about 1,100U/ml) was reacted with
antithrombin III
for 2 hr. The percent
thrombin
inactivated was then measured. In random samples of human blood, a wide range of
antithrombin III
concentration was found. The inhibitor is relatively stable in plasma and serum. It is not changed in concentration when Dicumarol therapy is instituted. Ether extraction of plasma reduces
antithrombin III
activity. Seitz filtration of plasma did not remove activity. Under special conditions,
antithrombin III
enhances esterase activity of
thrombin
. Under special conditions,
thrombin
regenerates from the
thrombin
-
antithrombin III
complex. Antithrombin III neutralizes the activity of prethrombin-E and
thrombin
-E; consequently, an active histidine center found in the B1 chain of
thrombin
is not essential for the binding of antithrombin. Autoprothrombin II-A activity was neutralized by
antithrombin III
. Autoprothrombin C was found to be neutralized by
antithrombin III
; the amounts required varied with the molecular forms of autoprothrombin C. Thrombin and autoprothrombin C apparently occupy the same binding sites on
antithrombin III
. An equation was developed to account for all the known characteristics of
antithrombin III
functions. The kinetic aspects of
thrombin
neutralization were found to correspond exactly with those of autoprothrombin C. Antithrombin III is a high-capacity inhibitor of the two most powerful enzymes in blood coagulation.
...
PMID:Antithrombin III: a backward glance o'er travel'd roads. 4 4
Antithrombin activity has been identified in intact washed human platelets. An apparent activity was demonstrated at platelet concentrations above 0.31 X 10(9)/ml, when platelet suspensions were incubated with 2.0 NIH units/ml of
thrombin
. Neither red cells nor white cells revealed antithrombin activity. No significant loss of the platelet antithrombin activity was observed after ten successive washings or after treatment of platelets with antibodies to
antithrombin III
or alpha2-macroglobulin. Almost the same amount of antithrombin activity as normal platelets was demonstrated in the platelets from an afibrinogenemic patient. Pre-treatment of platelets with trypsin, papain, and neuroaminidase reduced the activity significantly, whereas lipase was without effect. The platelet antithrombin reacted with
thrombin
in less than 3 seconds, and this rapid reaction of platelet antithrombin was different from that of plasma
antithrombin III
or fibrinogen. The
thrombin
-like clotting activity of ancrod was inhibited by fibrinogen but not platelets. Also, unlike plasma
antithrombin III
or fibrinogen, brief exposure to heat (56 degrees C or 60 degrees C) reduced considerable amounts of platelet antithrombin activity. These results suggest that platelets possess a specific antithrombin with different characteristics from other known antithrombins.
...
PMID:Antithrombin activity of intact human platelets. 5 97
A new rapid method for assaying total antithrombin activity has been developed based on the inactivation of
thrombin
incorporated into an agarose gel, during the radial diffusion of plasma in the gel. The area of
thrombin
inactivation is subsequently observed by the coagulation of fibrinogen in a separate agarose gel layer poured over the
thrombin
gel. The method is described in detail and its accuracy assessed with respect to other antithrombin assays. Using specific antisera to alpha2-globulin (
antithrombin III
), alpha2-macroglobin and alpha1-antitrypsin, total antithrombin activity measured by this assay consisted of 47% alpha2-globulin, 29% alpha2-macroglobulin and 26% alpha1-antitrypsin.
...
PMID:A new assay for the measurement of total progressive antithrombin. 5 64
A method for the differential determination of plasma antithrombins,
antithrombin III
and alpha2 macroglobulin, is described. The method is based on the selective inactivation of plasma alpha2 macroglobulin by treatment with 0-1 M methylamine for 10 minutes at 37 degrees C and on the observation that
antithrombin III
and alpha2 macroglobulin inhibited in defibrinated plasma low concentrations of
thrombin
without mutual interference and according to pseudo-first order reaction. In healthy subjects
antithrombin III
was shown to account for about 70% of the total antithrombin activity. But in patients with liver cirrhosis, where low levels of total antithrombin activity were observed, the relative contribution of
antithrombin III
was found to be noticeably lower.
...
PMID:A method for the differential determination of plasma antithrombins. 5 20
Antithrombin III, purified to homogeneity according to polyacrylamide gel disc electrophoresis and immunoelectrophoresis, inhibited the activity of purified factor IXa and Xa, whereas factor VII was not inhibited either in the active or in the native form. Antithrombin III is the single most important inhibitor of factor Xa in plasma. Factor Xa does not, however, reduce the activity of
antithrombin III
against
thrombin
.
...
PMID:The effect of antithrombin III on the activity of the coagulation factors VII, IX and X. 6 31
The
thrombin
time of normal citrated plasma is progressively prolonged on incubation in open glass tubes at 37 degrees C. The phenomenon is dependent on the temperature and duration of incubation, on the pH, and on the concentration of calcium ions present. Platelet-rich citrated plasma fails to exhibit augmented antithrombin activity when similarly incubated, and the addition of washed platelets to platelet-poor plasma inhibits this activity. The clot retarding action of incubated plasma against
thrombin
is also manifested against Arvin (Ancrod), but not against Reptilase-R. This
thrombin
time lengthening may be inhibited by incubation with anti-
antithrombin III
antiserum thus indicating that the phenomenon of
thrombin
time lengthening is consistent with enhanced activity of
antithrombin III
. It is unlikely that alterations in the activity of alpha2-macroglobulin, is important in the reduced
thrombin
-coagulability of incubated plasma. Interference with the polymerisation of fibrin monomers by the physico-chemical changes may contribute to the observed phenomenon.
...
PMID:The reversible antithrombin activity of incubated plasma. 6
The influence of hemofiltration on the number of platelets and on coagulation factors was investigated in patients with chronic renal insufficiency. These investigations were done on 12 patients during 22 treatments with hemofiltration. Blood samples were taken before hemofiltration, 10, 30 and 120 minutes after the beginning of the treatment and at the end of hemofiltration. In comparison to the original values we found a loss of platelets, a small decrease in the concentration of fibrinogen and a small increase in the fibrin monomer complex, plasminogen,
antithrombin III
, alpha1-antitrypsin and in alpha2-macroglobulin. The
thrombin
time, the partial thromboplastin time and Quick's test showed that the blood of these patients contained sufficient hepatin. Use of fibrin plates (Astrup) showed no signs of fibrinolytic activity. Compared to the results, which were obtained some years ago during hemodialysis, we found a smaller extent of alterations of blood coagulation factors and number of platelets.
...
PMID:Alterations of clotting factors and platelets during hemofiltration. 7 95
Human alpha-
thrombin
is inhibited by the circulating protease inhibitors alpha1-antitrypsin,
antithrombin III
, and alpha2-macroglobulin. Kinetic analyses of the inhibitor
thrombin
interactions were carried out utilizing either fibrinogen or the synthetic substrate Bz-Phe-Val-Arg-p-nitroanilide as substrates to determine residual
thrombin
activity. These studies demonstrated that the inhibition of
thrombin
by alpha1-antitrypsin,
antithrombin III
, and alpha2-macroglobulin followed second-order kinetics. The rate constants for the inhibition of
thrombin
by alpha1-antitrypsin,
antithrombin III
, and alpha2-macroglobulin are 6.51 +/- 0.38 x 10(3), 3.36 +/- 0.34 x 10(5), and 2.93 +/- 0.02 x 10(4) M-1 min-1, respectively. Comparison of the second-order rate constants and the normal plasma levels of the three inhibitors demonstrates that, under the in vitro conditions utilized,
antithrombin III
is five times and alpha2-macroglobulin is one-third as effective as alpha1-antitrypsin in the inhibition of
thrombin
.
...
PMID:Comparison of the inhibition of thrombin by three plasma protease inhibitors. 7 21
The interaction between
thrombin
and alpha-2-macroglobulin was studied on human purified materials, either in the presence or in the absence of heparin, by kinetic analysis of
thrombin
inhibition and polyacrylamide gel electrophoresis. In the absence of heparin, binding of
thrombin
to alpha-2-macroglobulin, shown by electrophoresis, leads to the loss of the coagulant property of the enzyme. In the presence of heparin the rate of inhibition of
thrombin
clotting activity by alpha-2-macroglobulin is strongly decreased. Heparin binds to
thrombin
, impairing the formation of
thrombin
-alpha-2-macroglobulin complex. These data show that heparin paradoxically protects
thrombin
from inhibition by alpha-2-macroglobulin whereas it increases the enzyme inhibition by
antithrombin III
. Such a phenomenon could be of practical interest for treatment of thrombosis in patients with high plasma level of alpha-2-macroglobulin and low level of
antithrombin III
, such as occurs in the nephrotic syndrome.
...
PMID:[Heparin inhibition of the antithrombin activity of alpha-2-macroglobulin]. 8 15
1
2
3
4
5
6
7
8
9
10
Next >>
