Characterization of ‘basparin A,’ a prothrombin-activating metalloproteinase, from the venom of the snake Bothrops asper that inhibits platelet aggregation and induces defibrination and thrombosis
| Autor: | R. David G. Theakston, Gilbert D. Loría, Alexandra Rucavado, Jay W. Fox, Aura S. Kamiguti, Alberto Alape, José María Gutiérrez |
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| Rok vydání: | 2003 |
| Předmět: |
Platelet Aggregation
Prothrombin Activator Biophysics Venom Pharmacology Biochemistry Sudden death Mice Prothrombinase Platelet Aggregation Inhibition Crotalid Venoms Animals Humans Defibrination Bothrops Molecular Biology Metalloproteinase biology Metalloendopeptidases Thrombosis biology.organism_classification Macroglobulin Bothrops Asper Venom Snake venom Immunology Platelet aggregation inhibitor Prothrombin Platelet Aggregation Inhibitors |
| Zdroj: | Archives of Biochemistry and Biophysics; Volumen 418, Número 1. 2003 Kérwá Universidad de Costa Rica instacron:UCR |
| ISSN: | 0003-9861 |
| DOI: | 10.1016/s0003-9861(03)00385-0 |
| Popis: | A prothrombin activator, named ‘basparin A,’ was isolated from the venom of the crotaline snake Bothrops asper, the species responsible for the majority of snakebite cases in Central America. It is an acidic (pI 5.4), 70 kDa, single chain P-III metalloproteinase comprising, in addition to the metalloproteinase domain, disintegrin-like, and high-cysteine domains. Basparin A is a glycoprotein displaying immunological cross-reactivity with BaH1, a P-III hemorrhagic metalloproteinase isolated from the same venom. It activates prothrombin through the formation of meizothrombin, without requiring additional cofactors; it is, therefore, a class A snake venom prothrombin activator. In contrast with most venom metalloproteinases, it does not degrade components of the extracellular matrix. Apart from its clotting activity, basparin A inhibits collagen-dependent platelet aggregation in vitro, an effect that does not depend on proteolytic activity. Clotting activity on human plasma is not abrogated by the plasma proteinase inhibitors α2 macroglobulin and murinoglobulin, whereas activity is completely inhibited by Costa Rican polyvalent (Crotalinae) anti-venom. Basparin A does not induce local tissue alterations, such as hemorrhage, myonecrosis, and edema, in mice. Moreover, it does not induce systemic hemorrhage, thrombocytopenia nor prolongation of the bleeding time following intravenous administration. At low doses, the only observed effect induced by basparin A, when injected intravenously or intramuscularly into mice, is defibrin(ogen)ation. At higher doses, intravenous administration resulted in sudden death due to numerous occluding thrombi in pulmonary vessels. Basparin A is likely to play an important role in the coagulopathy associated with B. asper envenoming. Universidad de Costa Rica/[741-A2-036]/UCR/Costa Rica Universidad de Costa Rica/741-A1-504]/UCR/Costa Rica Wellcome Trust/[062043]//Inglaterra International Foundation for Science/[2707-2]/IFS/Suecia UCR::Vicerrectoría de Investigación::Unidades de Investigación::Ciencias de la Salud::Instituto Clodomiro Picado (ICP) |
| Databáze: | OpenAIRE |
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