Purification and characterization of platelet aggregation inhibitor from the venom of Bitis arietans

O. Platonov, V. Nikulina, Y. Kucheryavyi, V. Gryshchuk, Y. Stohniy, V. Chernyshenko, O. Slominskyi, A. Rebriev, K. Savchenko, L. Garmanchuk
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Abstract

Disintegrins are the antagonists of integrin receptors that can be found mostly in snakes’ venom. They can inhibit platelet aggregation, thus preventing the formation of blood clots. By blocking the integrin receptors of cancer cells, disintegrins can inhibit proliferation and metastasis. Thus, the search for new sources of disintegrins and development of methods of their purification is an important task of modern biotechnolo­gy. This work was dedicated to the purification and characterization of inhibiting polypeptides from Bitis arietans­ venom. Crude venom of B. arietans was fractionated using ion-exchange chromatography on Q Sepharose followed by size-exclusion chromatography on Superdex 75 using FPLC method. Analysis of molecular weight of protein components was performed using SDS-PAGE and MALDI-TOF analysis on Voyager-DE. Aggregation of platelet-rich plasma (PRP) in the presence of platelet aggregation inhibitor was investigated using aggregometry on the AR2110. MTT test was used for measuring HeLa cells proliferation and survival in vitro. Two-step chromatography allowed us to obtain fraction that contained polypeptides possessing the dose-dependent inhibitory action on adenosine diphosphate (ADP)-induced platelet aggregation in PRP. SDS-PAGE showed that obtained fraction contained two polypeptides with molecular weight 9.0 and 13.67 kDa according­ to MALDI-TOF analysis. Purified polypeptides inhibited ADP-induced platelet aggregation with IC50 0.09 mg/ml. However, 0.005 mg/ml of fraction suppressed viability of HeLa cells according to MTT test on 20%. Discovered biological effects of fractions allowed us to conclude the possible use of these polypeptides as anti-aggregatory or anti-proliferative agents. Keywords: antithrombotic action, disintegrins, glycoprotein IIb/IIIa, platelets, snake venom
白斑双翅虫毒液中血小板聚集抑制剂的纯化及特性研究
崩解素是整合素受体的拮抗剂,主要存在于蛇毒中。它们可以抑制血小板聚集,从而防止血栓的形成。崩解素通过阻断癌细胞的整合素受体,抑制癌细胞的增殖和转移。因此,寻找崩解素的新来源和发展其纯化方法是现代生物技术的重要任务。本文研究了从黄斑双翅虫毒液中提取的抑制多肽的纯化和特性。采用Q Sepharose离子交换层析,Superdex 75高效液相色谱法进行分离纯化。在Voyager-DE上使用SDS-PAGE和MALDI-TOF分析蛋白质组分的分子量。在AR2110上应用聚集法研究富血小板血浆(PRP)在血小板聚集抑制剂存在下的聚集。采用MTT法检测HeLa细胞体外增殖和存活情况。两步色谱法使我们能够获得含有多肽的部分,这些多肽对PRP中二磷酸腺苷(ADP)诱导的血小板聚集具有剂量依赖性抑制作用。SDS-PAGE经MALDI-TOF分析,得到的部分含有分子量分别为9.0和13.67 kDa的多肽。纯化多肽抑制adp诱导的血小板聚集,IC50为0.09 mg/ml。MTT试验显示,0.005 mg/ml对20%的HeLa细胞有抑制作用。发现的生物效应分数使我们得出结论,这些多肽作为抗聚集或抗增殖剂的可能用途。关键词:抗血栓作用,崩解素,糖蛋白IIb/IIIa,血小板,蛇毒
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