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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 >Pharmacological properties and pathophysiological significance of a Kunitz-type protease inhibitor (Rusvikunin-II) and its protein complex (Rusvikunin complex) purified from Daboia russelii russelii venom
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Pharmacological properties and pathophysiological significance of a Kunitz-type protease inhibitor (Rusvikunin-II) and its protein complex (Rusvikunin complex) purified from Daboia russelii russelii venom

机译:从罗氏沼虾蛇毒中纯化的Kunitz型蛋白酶抑制剂(Rusvikunin-II)及其蛋白复合物(Rusvikunin复合物)的药理特性和病理生理学意义

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A 7.1 kDa basic peptide (Rusvikunin-II) was purified from a previously described protein complex (Rusvikunin complex, consists of Rusvikunin and Rusvikunin-II) of Daboia russelii russelii venom. The N-terminal sequence of Rusvikunin-II was found to be blocked, but peptide mass fingerprinting analysis indicated its identity as Kunitz-type basic protease inhibitor 2, previously reported from Russell's Viper venom. A tryptic peptide sequence of Rusvikunin-II containing the N-terminal sequence HDRPTFCNLFPESGR demonstrated significant sequence homology to venom basic protease inhibitors, Kunitz-type protease inhibitors and trypsin inhibitors. The secondary structure of Rusvikunin-II was dominated by beta-sheets (60.4%), followed by random coil (38.2%), whereas cc-helix (1.4%) contributes the least to its secondary structure. Both Rusvikunin-II and the Rusvikunin complex demonstrated dose-dependent anticoagulant activity; however, the anticoagulant potency of latter was found to be higher. Both inhibited the amidolytic activity of trypsin > plasmin FXa, fibrinogen clotting activity of thrombin, and, to a lesser extent, the prothrombin activation property of FXa; however, the inhibitory effect of the Rusvikunin complex was more pronounced. Neither Rusvikunin-II nor Rusvikunin complex inhibited the amidolytic activity of chymotrypsin and thrombin. Rusvikunin-II at 10 mu g/ml was not cytotoxic to Colo-205, MCF-7 or 3T3 cancer cells; conversely, Rusvikunin complex showed similar to 30% reduction of MCF-7 cells under identical experimental conditions. Rusvikunin-II (5.0 mg/kg body weight, i.p. injection) was not lethal to mice or House Geckos; nevertheless, it showed in vivo anticoagulant action in mice. However, the Rusvikunin complex (at 5.0 mg/kg) was toxic to NSA mice, but not to House Geckos, suggesting it has prey-specific toxicity. Rusvikunin complex-treated mice exhibited dyspnea and hind-limb paresis prior to death. The present study indicates that the Kunitz-type protein complex Rusvikunin from Russell's Viper venom significantly contributes to venom toxicity, and an important biological role in venoms appears to be facilitation of prey subjugation
机译:从先前描述的罗非鱼(Daboia russelii russelii)毒液的蛋白质复合物(Rusvikunin复合物,由Rusvikunin和Rusvikunin-II组成)中纯化了7.1kDa的碱性肽(Rusvikunin-II)。已发现Rusvikunin-II的N端序列被封闭,但肽质量指纹分析表明其与Kunitz型碱性蛋白酶抑制剂2相同,先前从Russell的Viper毒液中报道过。含有N末端序列HDRPTFCNLFPESGR的Rusvikunin-II的胰蛋白酶肽序列与毒液碱性蛋白酶抑制剂,Kunitz型蛋白酶抑制剂和胰蛋白酶抑制剂具有显着的序列同源性。 Rusvikunin-II的二级结构占主导地位的是β-折叠(60.4%),其次是无规卷曲(38.2%),而cc-螺旋(1.4%)对其二级结构的贡献最小。 Rusvikunin-II和Rusvikunin复合物均显示出剂量依赖性抗凝活性。然而,发现后者的抗凝效力更高。两者均抑制胰蛋白酶>纤溶酶 FXa的酰胺分解活性,抑制凝血酶的纤维蛋白原凝结活性,并在较小程度上抑制FXa的凝血酶原激活特性。然而,Rusvikunin复合物的抑制作用更为明显。 Rusvikunin-II和Rusvikunin复合物均不能抑制胰凝乳蛋白酶和凝血酶的酰胺分解活性。 Rusvikunin-II的浓度为10μg/ ml,对Colo-205,MCF-7或3T3癌细胞没有细胞毒性;相反,在相同的实验条件下,Rusvikunin复合物的MCF-7细胞减少了30%。 Rusvikunin-II(5.0 mg / kg体重,腹腔注射)对小鼠或家壁虎没有致死性。然而,它在小鼠中显示出体内抗凝作用。但是,Rusvikunin复合物(5.0 mg / kg)对NSA小鼠有毒性,对House Geckos没有毒性,表明它具有猎物特异性毒性。 Rusvikunin复合物治疗的小鼠在死亡前表现出呼吸困难和后肢轻瘫。本研究表明,来自罗素毒蛇毒液的Kunitz型蛋白复合物Rusvikunin显着促进了毒液的毒性,并且在毒液中的重要生物学作用似乎是促进了猎物的征服

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