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角蝰毒素,一种来自角蝰毒液的αβ纤维蛋白原酶,可激活纯化的凝血因子X并诱导人血小板释放5-羟色胺。

Afaâcytin, an alpha beta-fibrinogenase from Cerastes cerastes (horned viper) venom, activates purified factor X and induces serotonin release from human blood platelets.

作者信息

Laraba-Djebari F, Martin-Eauclaire M F, Mauco G, Marchot P

机构信息

Centre National de la Recherche Scientifique, Institut Fédératif de Recherche Jean Roche, Université d'Aix-Marseille II, France.

出版信息

Eur J Biochem. 1995 Nov 1;233(3):756-65. doi: 10.1111/j.1432-1033.1995.756_3.x.

DOI:10.1111/j.1432-1033.1995.756_3.x
PMID:8521839
Abstract

Afaâcytin, a proteinase with caseinolytic, arginine-esterase and amidase activities, was purified from the venom of Cerastes cerastes (horned viper) in two steps by gel filtration through Sephadex G75, then HPLC on carboxymethyl-cellulose. Afaâcytin has an isoelectric point of 6.25, and consists of two subunits, alpha and beta, which have the same apparent molecular mass (40,000) and are indistinguishable in the absence of reduction or/and deglycosylation. Subunit beta is constituted of two disulfide-linked polypeptidic chains, beta and beta'. The respective apparent molecular mass of the chains are 43,000 (alpha), 35,500 (beta) and 10,200 (beta') as determined by SDS/PAGE under reducing conditions. Both chains alpha and beta are N-glycosylated. The two chains have the same N-terminal sequence (20 residues) which is similar to those of other proteinases from snake venom. Susceptibility of afaâcytin to diisopropyl fluorophosphate and benzamidine indicates the presence of a serine and an aspartic (or glutamic) acid residues in the catalytic site. Ca2+ appears to be required for structural cohesion of the afaâcytin molecule. Afaâcytin exhibits alpha beta-fibrinogenase and alpha-fibrinase properties. It replaces missing factors VIII and IX in deficient plasmas, and activates purified human factor X into factor Xa. It releases serotonin from platelets and directly aggregates human (but not rabbit) blood platelets. Despite its thrombin-like characteristics, however, afaâcytin is not inhibited by plasmatic thrombin inhibitors. The procoagulant properties of afaâcytin therefore have potential clinical applications.

摘要

阿法西丁是一种具有酪蛋白水解、精氨酸酯酶和酰胺酶活性的蛋白酶,通过Sephadex G75凝胶过滤,然后在羧甲基纤维素上进行高效液相色谱,分两步从角蝰蛇毒中纯化得到。阿法西丁的等电点为6.25,由α和β两个亚基组成,这两个亚基具有相同的表观分子量(40,000),在未进行还原或/和去糖基化时无法区分。亚基β由两条通过二硫键连接的多肽链β和β'组成。在还原条件下通过SDS/PAGE测定,各条链的表观分子量分别为43,000(α)、35,500(β)和10,200(β')。α和β两条链均为N - 糖基化。两条链具有相同的N端序列(20个残基),与其他蛇毒蛋白酶的序列相似。阿法西丁对二异丙基氟磷酸和苯甲脒的敏感性表明其催化位点存在一个丝氨酸和一个天冬氨酸(或谷氨酸)残基。钙离子似乎是阿法西丁分子结构凝聚所必需的。阿法西丁具有αβ - 纤维蛋白原酶和α - 纤维蛋白酶特性。它能替代缺陷血浆中缺失的因子VIII和IX,并将纯化的人因子X激活为因子Xa。它能从血小板中释放5 - 羟色胺,并直接聚集人(而非兔)血小板。然而,尽管阿法西丁具有类似凝血酶的特性,但它不受血浆凝血酶抑制剂的抑制。因此,阿法西丁的促凝血特性具有潜在的临床应用价值。

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