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首页> 外文期刊>Toxicon: An International Journal Devoted to the Exchange of Knowledge on the Poisons Derived from Animals, Plants and Microorganisms >Agkihpin, a novel SVTLE from Gloydius halys Pallas, promotes platelet aggregation in vitro and inhibits thrombus formation in vivo in murine models of thrombosis
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Agkihpin, a novel SVTLE from Gloydius halys Pallas, promotes platelet aggregation in vitro and inhibits thrombus formation in vivo in murine models of thrombosis

机译:Agkihpin,一种来自Gloydius halys Pallas的新型SVTLE,在血栓形成的小鼠模型中,在体外促进血小板聚集并在体内抑制血栓形成

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In previous work, a snake venom arginine esterase (SVAE), agkihpin from the venom of Gloydius halys Pallas, was isolated and its biochemical data including Mr, PI, amino acid components and sugar content was collected. Here, the agkihpin was cloned and further characterized and we found that agkihpin could promote ADP-induced platelets aggregation, hydrolyze fibrin, cleave A alpha and B beta chains of fibrinogen and reduce the thrombosis induced by thrombin. Moreover, agkihpin hydrolyzed TAME with optimum temperatures at 30 degrees C-45 degrees C, and the hydrolysis was inhibited by EDTA, PMSF, DTT and promoted by Ca2+, Fe3+, Mg2+, Zn2+. The sequence features of agkihpin were detected as follows: the N-terminal residues was determined as I(V)L(Y)GDDECNINE by protein sequencing; the ORF was determined as 705 bp, and the deduced amino acid sequence was identified by peptide mass fingerprinting; the cysteines, cleavage sites, active sites and substrate binding sites of snake venom thrombin-like enzyme (SVTLE), were all conserved in amino acid sequence of agkihpin; 2 Leu(Tyr), 4 Asn and 121 Ile in amino acid sequence of agkihpin were first found in the amino acid sequences of SVTLEs. These findings indicated that agkihpin is a novel SVTLE. What's more, due to its several advantages of fibrino(gen)olytic and thrombosis-reduced activities, and devoid of bleeding risk, agkihpin may be developed into a thrombolytic drug in the future. (C) 2016 Elsevier Ltd. All rights reserved.
机译:在以前的工作中,蛇毒蛇毒精氨酸酯酶(SVAE),从Gloydius halys Pallas的蛇毒中分离出来,并收集了其生化数据,包括Mr,PI,氨基酸成分和糖含量。在这里,agkihpin被克隆并进一步表征,我们发现agkihpin可以促进ADP诱导的血小板聚集,水解纤维蛋白,切割纤维蛋白原的Aα和Bβ链并减少凝血酶引起的血栓形成。此外,agkihpin在30-45℃的最佳温度下水解TAME,EDTA,PMSF,DTT抑制了水解,而Ca2 +,Fe3 +,Mg2 +,Zn2 +促进了水解。 agkihpin的序列特征检测如下:通过蛋白质测序确定N-末端残基为I(V)L(Y)GDDECNIN​​E。确定ORF为705 bp,通过肽质量指纹图谱鉴定推导的氨基酸序列。蛇毒凝血酶样酶(SVTLE)的半胱氨酸,切割位点,活性位点和底物结合位点均在agkihpin的氨基酸序列中保守。首先在SVTLE的氨基酸序列中发现了agkihpin的氨基酸序列中的2 Leu(Tyr),4 Asn和121 Ile。这些发现表明,agkihpin是一种新颖的SVTLE。此外,由于其具有纤维蛋白水解和血栓形成减少活动的多个优点,并且没有出血风险,因此未来可能会开发出agkihpin成为溶栓药物。 (C)2016 Elsevier Ltd.保留所有权利。

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