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抑制因子VII-组织因子复合物的脂蛋白相关凝血抑制剂也能抑制因子Xa:对其可能作用机制的深入了解。

The lipoprotein-associated coagulation inhibitor that inhibits the factor VII-tissue factor complex also inhibits factor Xa: insight into its possible mechanism of action.

作者信息

Broze G J, Warren L A, Novotny W F, Higuchi D A, Girard J J, Miletich J P

机构信息

Division of Hematology/Oncology, Washington University School of Medicine, Jewish Hospital, St Louis, MO 63110.

出版信息

Blood. 1988 Feb;71(2):335-43.

PMID:3422166
Abstract

Blood coagulation is initiated when plasma factor VII(a) binds to its essential cofactor tissue factor (TF) and proteolytically activates factors X and IX. Progressive inhibition of TF activity occurs upon its addition to plasma. This process is reversible and requires the presence of VII(a), catalytically active Xa, Ca2+, and another component that appears to be associated with the lipoproteins in plasma, a lipoprotein-associated coagulation inhibitor (LACI). A protein, LACI(HG2), possessing the same inhibitory properties as LACI, has recently been isolated from the conditioned media of cultured human liver cells (HepG2). Rabbit antisera raised against a synthetic peptide based on the N-terminal sequence of LACI(HG2) and purified IgG from a rabbit immunized with intact LACI(HG2) inhibit the LACI activity in human serum. In a reaction mixture containing VIIa, Xa, Ca2+, and purified LACI(HG2), the apparent half-life (t1/2) for TF activity was 20 seconds. The presence of heparin accelerated the initial rate of inhibition threefold. Antithrombin III alpha alone had no effect, but antithrombin III alpha with heparin abrogated the TF inhibition. LACI(HG2) also inhibited Xa with an apparent t1/2 of 50 seconds. Heparin enhanced the rate of Xa inhibition 2.5-fold, whereas phospholipids and Ca2+ slowed the reaction 2.5-fold. Xa inhibition was demonstrable with both chromogenic substrate (S-2222) and bioassays, but no complex between Xa and LACI(HG2) could be visualized by sodium dodecyl sulfate-polyacrylamide gel electrophoresis (SDS-PAGE). Nondenaturing PAGE, however, showed that LACI(HG2) bound to Xa but not to X or Xa inactivated by diisopropyl fluorophosphate. Thus, LACI(HG2) appears to bind to Xa at or near its active site. Bovine factor Xa lacking its gamma-carboxyglutamic acid-containing domain, BXa(-GD), through treatment with alpha-chymotrypsin, was used to further investigate the Xa requirement for VIIa/TF inhibition by LACI(HG2). LACI(HG2) bound to BXa(-GD) and inhibited its catalytic activity against a small molecular substrate (Spectrozyme Xa), though at a rate approximately sevenfold slower than native BXa. Preincubation of LACI(HG2) with saturating concentrations of BXa(-GD) markedly retarded the subsequent inhibition of BXa. The VII(a)/TF complex was not inhibited by LACI(HG2) in the presence of BXa(-GD), and further, preincubation of LACI(HG2) with BXa(-GD) slowed the inhibition of VIIa/TF after the addition of native Xa. The results are consistent with the hypothesis that inhibition of VII(a)/TF involves the formation of a VIIa-TF-XA-LACI complex that requires the GD of XA.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

当血浆因子VII(a)与其必需辅因子组织因子(TF)结合并蛋白水解激活因子X和IX时,血液凝固启动。将TF添加到血浆中会导致TF活性逐渐受到抑制。此过程是可逆的,并且需要VII(a)、具有催化活性的Xa、Ca2+以及另一种似乎与血浆中的脂蛋白相关的成分,即脂蛋白相关凝血抑制剂(LACI)的存在。一种与LACI具有相同抑制特性的蛋白质LACI(HG2),最近已从培养的人肝细胞(HepG2)的条件培养基中分离出来。针对基于LACI(HG2) N端序列的合成肽产生的兔抗血清,以及用完整的LACI(HG2)免疫的兔纯化的IgG,均可抑制人血清中的LACI活性。在含有VIIa、Xa、Ca2+和纯化的LACI(HG2)的反应混合物中,TF活性的表观半衰期(t1/2)为20秒。肝素的存在使初始抑制速率加快了三倍。单独的抗凝血酶IIIα没有作用,但抗凝血酶IIIα与肝素一起可消除TF抑制作用。LACI(HG2)也以50秒的表观t1/2抑制Xa。肝素使Xa抑制速率提高了2.5倍,而磷脂和Ca2+使反应减慢了2.5倍。用发色底物(S-2222)和生物测定法均可证明Xa受到抑制,但通过十二烷基硫酸钠-聚丙烯酰胺凝胶电泳(SDS-PAGE)无法观察到Xa与LACI(HG2)之间形成复合物。然而,非变性PAGE显示LACI(HG2)与Xa结合,但不与经二异丙基氟磷酸灭活的X或Xa结合。因此,LACI(HG2)似乎在Xa的活性位点或其附近与之结合。通过用α-胰凝乳蛋白酶处理,去除了含γ-羧基谷氨酸结构域的牛因子Xa,即BXa(-GD),用于进一步研究LACI(HG2)对VIIa/TF抑制的Xa需求。LACI(HG2)与BXa(-GD)结合并抑制其对小分子底物(光谱酶Xa)的催化活性,尽管其速率比天然BXa慢约七倍。用饱和浓度的BXa(-GD)对LACI(HG2)进行预孵育,可显著延迟随后对BXa的抑制。在存在BXa(-GD)的情况下,LACI(HG2)不会抑制VII(a)/TF复合物,此外,在加入天然Xa后,用BXa(-GD)对LACI(HG2)进行预孵育会减慢对VIIa/TF的抑制。这些结果与以下假设一致,即VII(a)/TF的抑制涉及形成VIIa-TF-XA-LACI复合物,该复合物需要XA的GD。(摘要截短为400字)

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