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新生儿抗凝血酶III的生化与功能研究

Biochemical and functional study of antithrombin III in newborn infants.

作者信息

McDonald M M, Hathaway W E, Reeve E B, Leonard B D

出版信息

Thromb Haemost. 1982 Feb 26;47(1):56-8.

PMID:7071806
Abstract

Antithrombin III (AT-III) was isolated by heparin affinity chromatography from adult venous and newborn term and preterm umbilical cord blood. The purified proteins were compared by SDS-PAGE, rocket immuno-electrophoresis, protein concentration by microbiuret relative to optical density at 280 nm, heparin cofactor specific activity, progressive neutralization of thrombin and factor Xa at 37 degree C and pH related antithrombin kinetics. The structural evaluations revealed a fetal AT-III of molecular weight, charge and electrophoretic migration indistinguishable from adult AT-III. The functional studies showed that, on an equimolar basis, the rates of thrombin and Xa interactions with fetal AT-III were as rapid as those with adult AT-III. The catalytic rates of various concentrations of heparin were also equal. The newborn infant, therefore, displays a quantitative but not quantitative deficiency of AT-III.

摘要

通过肝素亲和层析从成人静脉血、足月新生儿和早产新生儿脐带血中分离出抗凝血酶III(AT-III)。采用十二烷基硫酸钠-聚丙烯酰胺凝胶电泳(SDS-PAGE)、火箭免疫电泳、通过缩二脲法相对于280nm光密度测定蛋白质浓度、肝素辅因子比活性、在37℃和pH条件下对凝血酶和因子Xa的逐步中和以及与抗凝血酶动力学相关的pH值,对纯化后的蛋白质进行比较。结构评估显示,胎儿AT-III的分子量、电荷和电泳迁移率与成人AT-III无法区分。功能研究表明,在等摩尔基础上,凝血酶和Xa与胎儿AT-III相互作用的速率与它们与成人AT-III相互作用的速率一样快。不同浓度肝素的催化速率也相等。因此,新生儿显示出AT-III存在定量而非定性缺陷。

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