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纯合子蛋白C缺乏症:关于分子异常性质及华法林治疗效果的观察

Homozygous protein C deficiency: observations on the nature of the molecular abnormality and the effectiveness of warfarin therapy.

作者信息

Peters C, Casella J F, Marlar R A, Montgomery R R, Zinkham W H

机构信息

Department of Pediatrics, Johns Hopkins School of Medicine, Baltimore, MD.

出版信息

Pediatrics. 1988 Feb;81(2):272-6.

PMID:3340476
Abstract

An infant with severe homozygous protein C deficiency was brought to medical attention because of purpura fulminans and severe bilateral vitreous hemorrhages in the neonatal period. Infusions of fresh frozen plasma were given for 8 months. On two occasions, attempts to decrease the frequency of fresh frozen plasma infusions to less than twice a day led to episodes of microangiopathic hemolysis, fibrinolysis, and acute renal failure. Infarction of skin and subcutaneous tissues did not recur. Both episodes were controlled after reinstitution of fresh frozen plasma. Complications of therapy with fresh frozen plasma included hyperproteinemia and hypertension. Warfarin therapy was instituted when the baby was 8 months of age, followed by a gradual withdrawal of fresh frozen plasma therapy. The dose of warfarin required to maintain the prothrombin time in a range of 1.8 to 2.2 times normal varied considerably during short periods, a phenomenon that may have been due to several factors: hypercatabolism of the drug with prolonged administration, abnormality of liver function, variation in levels of serum albumin, fluctuations in drug dosage secondary to oral administration, and variations in dietary vitamin K. Protein C determinations by immunologic and functional assays consistently showed detectable but reduced protein C antigen levels with undetectable activity levels, suggesting that a dysproteinemia rather than a deficiency of synthesis is responsible for the child's coagulopathy.

摘要

一名患有严重纯合子蛋白C缺乏症的婴儿在新生儿期因暴发性紫癜和严重双侧玻璃体出血而引起医疗关注。输注新鲜冰冻血浆持续了8个月。有两次,试图将新鲜冰冻血浆输注频率降低至每天少于两次,导致了微血管病性溶血、纤维蛋白溶解和急性肾衰竭发作。皮肤和皮下组织梗死未再复发。重新输注新鲜冰冻血浆后,两次发作均得到控制。新鲜冰冻血浆治疗的并发症包括高蛋白血症和高血压。婴儿8个月大时开始使用华法林治疗,随后逐渐停用新鲜冰冻血浆治疗。在短时间内,将凝血酶原时间维持在正常范围1.8至2.2倍所需的华法林剂量变化很大,这种现象可能是由多种因素导致的:长期给药导致药物分解代谢增加、肝功能异常、血清白蛋白水平变化、口服给药后药物剂量波动以及饮食中维生素K的变化。通过免疫和功能测定的蛋白C测定结果一致显示,蛋白C抗原水平可检测但降低,活性水平无法检测,这表明是异常蛋白血症而非合成不足导致了患儿的凝血病。

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