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肝素在新生儿血浆中的抗凝作用。

Anticoagulant effects of heparin in neonatal plasma.

作者信息

Schmidt B, Ofosu F A, Mitchell L, Brooker L A, Andrew M

机构信息

Department of Pediatrics, McMaster University, Hamilton, Ontario, Canada.

出版信息

Pediatr Res. 1989 Apr;25(4):405-8. doi: 10.1203/00006450-198904000-00020.

Abstract

Available data on the anticoagulant effects of heparin in neonatal plasma are scarce and conflicting: relative to adult plasma, neonatal plasma has been reported to show both resistance as well as sensitivity to heparin. We explored this apparent paradox by comparing how well heparin accelerated inhibition of exogenous thrombin and prevented thrombin generation in defibrinated neonatal and adult plasmas. Using amidolytic assays, we determined the effects of heparin on 1) the neutralization of exogenous human alpha-thrombin and on 2) the formation of endogenous thrombin activity after contact activation and recalcification. Neonatal plasma proved resistant to heparin (0.05 U/mL) during inhibition of added thrombin (15 NIH U/mL). Inhibition of thrombin in heparinized neonatal plasma became as efficient as in adult plasma only after raising the AT III activity to normal adult values. However, de novo generation of thrombin activity was very susceptible to inhibition by heparin, even in neonatal plasmas with physiologically low AT III levels. Peak thrombin activity generated in neonatal plasma in the absence of heparin was 50% or less of peak adult activity, and this already reduced ability of neonatal plasma to generate thrombin activity upon prothrombin activation was further decreased by heparin (0.05-0.2 U/mL). We conclude that due to the neonatal AT III deficiency, added thrombin is inactivated less effectively by heparin in neonatal than in normal adult plasma. Yet, the generation of thrombin activity is impaired in neonatal plasma and easily suppressed by heparin. We speculate that newborn infants may be resistant to heparin therapy during overt thrombotic disease, when neutralization of abnormal thrombin activity is the therapeutic goal.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

关于肝素在新生儿血浆中的抗凝作用的现有数据稀少且相互矛盾

与成人血浆相比,据报道新生儿血浆对肝素既表现出抵抗性又表现出敏感性。我们通过比较肝素在去纤维蛋白的新生儿和成人血浆中加速对外源凝血酶的抑制以及防止凝血酶生成的效果,来探究这一明显的矛盾。使用酰胺水解测定法,我们确定了肝素对1)外源性人α-凝血酶的中和作用以及2)接触激活和重新钙化后内源性凝血酶活性形成的影响。在抑制添加的凝血酶(15 NIH U/mL)期间,新生儿血浆对肝素(0.05 U/mL)表现出抵抗性。只有将抗凝血酶III(AT III)活性提高到正常成人水平后,肝素化新生儿血浆中凝血酶的抑制才变得与成人血浆一样有效。然而,即使在生理上AT III水平较低的新生儿血浆中,凝血酶活性的从头生成也非常容易受到肝素的抑制。在没有肝素的情况下,新生儿血浆中产生的凝血酶活性峰值是成人峰值的50%或更低,并且在凝血酶原激活时,新生儿血浆中这种已经降低的凝血酶活性生成能力会因肝素(0.05 - 0.2 U/mL)而进一步降低。我们得出结论,由于新生儿AT III缺乏,与正常成人血浆相比,肝素在新生儿中对外源添加凝血酶的灭活效果较差。然而,新生儿血浆中凝血酶活性的生成受损,并且容易被肝素抑制。我们推测,当以中和异常凝血酶活性为治疗目标时,新生儿在明显的血栓性疾病期间可能对肝素治疗有抵抗性。(摘要截断于250字)

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