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吸血蝙蝠(圆叶吸血蝠)唾液中抗凝因子——吸血蝙蝠素的纯化及部分特性分析

Purification and partial characterization of draculin, the anticoagulant factor present in the saliva of vampire bats (Desmodus rotundus).

作者信息

Apitz-Castro R, Béguin S, Tablante A, Bartoli F, Holt J C, Hemker H C

机构信息

Instituto Venezolano de Investigaciones Cientificas (IVIC), Caracas.

出版信息

Thromb Haemost. 1995 Jan;73(1):94-100.

PMID:7740503
Abstract

From the saliva of the vampire bat Desmodus rotundus, we isolated an unknown anticoagulant protein which we have named draculin. Its molecular mass as determined by non-reduced SDS-PAGE is about 83 kDa. The reduced polypeptide shows a slower migration. HPLC in a molecular sieve matrix yields a single, symmetrical peak corresponding to 88.5 kDa. Isoelectric focusing shows an acidic protein with pI = 4.1-4.2. Aminoacid analysis is compatible with a single chain polypeptide of about 80 kDa. Cyanogen bromide cleavage yields a single 16-aminoacid peptide, corresponding to the amino-terminus of the native molecule. Draculin inhibits the activated form of coagulation factors IX and X. It does not act on thrombin, trypsin, chymotrypsin and does not express fibrinolytic activity. The inhibition is immediate and not readily reversible, with a stoichiometry of about two molecules of draculin per molecule of factor IXa or Xa. Surprisingly, the inhibitory activity against either factor is not affected by the presence of the other. Draculin binds quantitatively to either immobilised factor Xa or factor IXa. Our preliminary interpretation is that there are two forms of draculin that hardly differ in structure. Both bind to factor Xa and to factor IXa but one form inhibits factor Xa and the other inhibits factor IXa. When added to plasma, draculin increases the lag phase as well as the height of the peak of thrombin generation.

摘要

从吸血蝙蝠圆叶吸血蝠的唾液中,我们分离出一种未知的抗凝血蛋白,我们将其命名为吸血素。通过非还原SDS-PAGE测定,其分子量约为83 kDa。还原后的多肽迁移速度较慢。在分子筛基质中进行HPLC分析得到一个单一的对称峰,对应分子量为88.5 kDa。等电聚焦显示该蛋白为酸性蛋白,pI = 4.1 - 4.2。氨基酸分析表明它是一条约80 kDa的单链多肽。溴化氰裂解产生一个由16个氨基酸组成的单一肽段,对应于天然分子的氨基末端。吸血素能抑制凝血因子IX和X的活化形式。它对凝血酶、胰蛋白酶、糜蛋白酶无作用,也不表现出纤溶活性。这种抑制作用是即时的且不易逆转,化学计量比约为每分子IXa或Xa对应两分子吸血素。令人惊讶的是,对任一因子的抑制活性不受另一种因子存在的影响。吸血素能与固定化的因子Xa或因子IXa定量结合。我们初步的解释是,吸血素有两种结构几乎无差异的形式。两者都能结合因子Xa和因子IXa,但一种形式抑制因子Xa,另一种抑制因子IXa。当添加到血浆中时,吸血素会延长凝血酶生成的延迟期并增加其峰值高度。

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