首页> 外文期刊>Biochimica et biophysica acta: BBA: International journal of biochemistry, biophysics and molecular biololgy. Proteins and Proteomics >A novel serine protease with human fibrino(geno)lytic activities from Artocarpus heterophyllus latex
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A novel serine protease with human fibrino(geno)lytic activities from Artocarpus heterophyllus latex

机译:一种来自面包果乳胶的具有人纤维蛋白溶酶活性的新型丝氨酸蛋白酶

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摘要

A protease was isolated and purified from Artocarpus heterophyllus (jackfruit) latex and designated as a 48-kDa antimicrobial protease (AMP48) in a previous publication. In this work, the enzyme was characterized for more biochemical and medicinal properties. Enzyme activity of AMP48 was strongly inhibited by phenylmethanesulfonyl fluoride and soybean trypsin inhibitor, indicating that the enzyme was a plant serine protease. The N-terminal amino acid sequences (A-Q-E-G-G-K-D-D-D-G-G) of AMP48 had no sequence similarity matches with any sequence databases of BLAST search and other plant serine protease. The secondary structure of this enzyme was composed of high α-helix (51%) and low β-sheet (9%). AMP48 had fibrinogenolytic activity with maximal activity between 55 and 60 °C at pH 8. The enzyme efficiently hydrolyzed α followed by partially hydrolyzed β and γ subunits of human fibrinogen. In addition, the fibrinolytic activity was observed through the degradation products by SDS-PAGE and emphasized its activity by monitoring the alteration of secondary structure of fibrin clot after enzyme digestion using ATR-FTIR spectroscopy. This study presented the potential role to use AMP48 as antithrombotic for treatment thromboembolic disorders such as strokes, pulmonary emboli and deep vein thrombosis.
机译:从面包果(菠萝蜜)胶乳中分离并纯化了一种蛋白酶,在以前的出版物中将其命名为48 kDa抗菌蛋白酶(AMP48)。在这项工作中,该酶具有更多的生化和药用特性。苯甲磺酰氟和大豆胰蛋白酶抑制剂强烈抑制AMP48的酶活性,表明该酶是植物的丝氨酸蛋白酶。 AMP48的N端氨基酸序列(A-Q-E-G-G-K-D-D-D-G-G)与BLAST搜索和其他植物丝氨酸蛋白酶的任何序列数据库都没有序列相似性匹配。该酶的二级结构由高α-螺旋(51%)和低β-折叠(9%)组成。 AMP48具有纤维蛋白原分解活性,在pH值为8时在55至60°C之间具有最大活性。该酶有效地水解了人类纤维蛋白原的α,然后部分水解了β和γ亚基。另外,通过SDS-PAGE通过降解产物观察到了纤溶活性,并通过使用ATR-FTIR光谱监测酶消化后血纤蛋白凝块的二级结构的变化来强调其活性。这项研究提出了使用AMP48作为抗血栓药治疗血栓栓塞性疾病(如中风,肺栓塞和深静脉血栓形成)的潜在作用。

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