Übersetzung für "Kininogen" in Deutsch

Bradykinin is produced from the high molecular weight kininogen.

Fitzgerald Trait Plasma is a lyophilized and stabilized human high molecular weight kininogen deficient plasma.

By splitting two peptide bonds, it liberates the pharmacologically extremely active kinins only from the glycoprotein which occurs in the globulin fraction of serum and is called kininogen.

Attempts to remove proteolytic enzymes by adsorption on bentonite, silica gel, barium sultate, active carbon, or affinity exchangers have not succeeded in eliminating all the deleterious proteases and, depending on the method of manufacturing the immunoglobulin-G preparation, immunological and enzymatic tests have shown it still to contain varying levels of prekallikrein, kininogen and kallikrein even when the presence of any significant level of prekallikrein activator was impossible to identify.

It has surprisingly now been discovered that concentrations of 0.4 to I.5% by volume and preferably of 0.8 to 1.0% by volume of octanoic acid can be employed to eliminate specifically proteolytic enzymes and such compounds as prekallikrein, kallikrein and kininogen that trigger vasoactive reactions, from previously purified immunoglobulin-G solutions with no significant precipitation of protein.

Further preferred examples relate to preparations with antibodies against procoagulants (blood coagulation factors II, V, VII, IX, X, XI, XII, prekallikrein, kininogen and tissue factor), but also preparations with antibodies against anticoagulants (protein C, protein S, antithrombin III, heparin cofactor II), clot structure factors (fibrinogen and factor XIII), fibrinolysis factors (plasminogen, t-PA, PAI-1 and a2 -plasmin inhibitor) and phospholipids.

We have examined tissues from human abdominal aortic aneurysm and found an activation of matrix metalloproteases, cystein proteases, and components of the renin-angiotensin system (cathepsin D, chymase, AT1 receptor) as well as down-regulation of the anti-proteolytic mediators (TIMP-4 and high molecular weight kininogen).

Thus, PK can, by means of proteolytic cleavage, liberate the vasoactive peptide bradykinin from high molecular weight kininogen and activate the proteases coagulation factor XII, prourokinase, plasminogen and Pro-MMP 3.

Thus, PK is able to release by proteolytic cleavage the vasoactive peptide bradykinin from high molecular weight kininogen and to activate the zymogens coagulation factor XII, pro-urokinase, plasminogen and pro-MMP 3.

The intrinsic pathway is initiated when prekallikrein, high molecular weight kininogen factor XI and XII bind to a negatively charged surface.

The intrinsic pathway requires the clotting factors V, VIII, IX, X, XI and XII and also prekallikrein, high molecular weight kininogen, calcium ions and phospholipids from platelets.

The intrinsic pathway requires coagulation factors VIII, IX, X, XI and XII and prekallikrein, high molecular weight kininogen, calcium ions and phospholipids from platelets.

Hyperpermeability of the monolayer formed is induced by stimulation with kininogen, prekallikrein and factor XII (100 nM each).

Hyperpermeability of the monolayer is induced by stimulation with kininogen, prekallikrein and factor XII (100 nM each).

On the surface, initially factor XII is activated to factor XIIa which subsequently, via kininogen or glycoprotein Ib, activates factor XI attached to cell surfaces.

Hyperpermeability of the confluent cell monolayer formed is induced by stimulation with kininogen, prekallikrein and factor XII (100 nM each).

The intrinsic pathway requires coagulation factors VIII, IX, X, XI and XII and also prekallikrein, high molecular weight kininogen, calcium ions and phospholipids from platelets.

The intrinsic pathway is initiated when prekallikrein, high molecular weight kininogen, factor XI and XII bind to a negatively charged surface.

Using primary cell cultures (VSMC, EC), we could also demonstrate that two chain high molecular weight kininogen decreases MMP-2 expression induced by interleukin-1alpha in VSMC and prevents apoptosis.