G I Nikonov scite author profile

Electrophoretic analysis of destabilase preparation demonstrates the presence of protein combinations with MW 12.3, 25 and 50 kD. Fraction (MW 12.3 D) is a monomer of destabilase aggregation having properties of micellar proteins and represents a stable lipid-protein complex, where the role of lipid component is played by the stable analogue of prostacyclin (MW 391 D). The synthesis of a low molecular fraction of destabilase is fulfilled with bacteria--symbiont of leeches Aeromonas hydrophila. When the destabilase (MW 12.3 kD) contacts with blood a process of complexe formation is triggered with hirudin and blood plasma kallikrein inhibitor, forming a stable 'destabilase complex' (DC; MW 25 kD), possessing also a high aggregation capacity. Polymer forms of the destabilase complex form a liposome changing its spatial orientation depending on the nature of the solvent. Such structural organization provides a high stability of DC components and a rapid penetration through cellular membranes (transmembrane transfer) and it also provides prophylactic antithrombotic action in the case of peroral application to animals, due to the blockade of vascular platelets (inhibition of platelet aggregation by prostacyclin analogue) and plasmic (inhibition of thrombin activity and blood plasma kallikrein) links of the hemostasis process. Destabilase fraction with MW 50 kD is a dimer of the destabilase complex. As a result of DC destruction (liposome), hirudin, prostacycline analogue and blood plasma kallikrein inhibitor are released.

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Biological activity and pharmacological properties of anticoagulant complex (Hirudin, plasma kallikrein inhibitor, prostaglandin) fromHirudo Medicinalis

Nikonov

Титова

Seleznev

1999

Bull Exp Biol Med

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Antiprocoagulant complex isolated from lyophilized medicinal leeches exerted pronounced antithrombotic, thrombolytic, and hypotensive effects in experimental animals after intravenous injection and showed antithrombotic activity after oral administration in combination with hirudone, the source of hyaluronidase and inhibitors of digestive proteolytic enzymes, The antiprocoagulant complex can be used as a specific medicinal preparation.

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Effect of the salivary gland secretion ofHirudo medicinalis on the extrinsic and intrinsic mechanisms of blood clotting

Baskova¹,

Khalil²,

Nikonov³

1984

Bull Exp Biol Med

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G I Nikonov

Destabilase, the novel ϵ-(??-Glu)-Lys isopeptidase with thrombolytic activity

A stable prostacyclin-like substance produced by the medicinal leech Hirudo medicinalis

Destabilase complexes ‐ natural liposome produced by medicinal leeches Hirudo medicinalis

Biological activity and pharmacological properties of anticoagulant complex (Hirudin, plasma kallikrein inhibitor, prostaglandin) fromHirudo Medicinalis

Effect of the salivary gland secretion ofHirudo medicinalis on the extrinsic and intrinsic mechanisms of blood clotting

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G I Nikonov

Destabilase, the novel &epsiv;-(??-Glu)-Lys isopeptidase with thrombolytic activity

A stable prostacyclin-like substance produced by the medicinal leech Hirudo medicinalis

Destabilase complexes ‐ natural liposome produced by medicinal leeches Hirudo medicinalis

Biological activity and pharmacological properties of anticoagulant complex (Hirudin, plasma kallikrein inhibitor, prostaglandin) fromHirudo Medicinalis

Effect of the salivary gland secretion ofHirudo medicinalis on the extrinsic and intrinsic mechanisms of blood clotting

Contact Info

Product

Resources

About

Destabilase, the novel ϵ-(??-Glu)-Lys isopeptidase with thrombolytic activity