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健康人类胎儿血液凝固激活剂和抑制剂的演变

Evolution of blood coagulation activators and inhibitors in the healthy human fetus.

作者信息

Reverdiau-Moalic P, Delahousse B, Body G, Bardos P, Leroy J, Gruel Y

机构信息

Laboratoire d'Hématologie-Hémostas Foetale, Groupe Interactions Hôte-Greffon, Faculté de Médecine, Tours, France.

出版信息

Blood. 1996 Aug 1;88(3):900-6.

PMID:8704247
Abstract

Blood coagulation proteins were determined in 285 healthy fetuses from 19 to 38 weeks' gestation and compared with those of 60 normal full-term newborns and 40 adult controls. Prolongation of the coagulation screening tests, prothrombin time, activated partial prothrombin time, and thrombin clotting time, in fetuses throughout intrauterine life was explained by low levels of vitamin K-dependent factors (II, VII, IX, and X), contact factors (XI, XII, prekallikrein, and high-molecular-weight kininogen), factor V, factor VIII, and fibrinogen. Low levels of antithrombin III, heparin cofactor II, protein C and protein S, and tissue factor pathway inhibitor were also found, and these probably contributed to a satisfactory hemostatic balance. Some of these parameters were evaluated by both immunologic and functional assays to detect possible "fetal" proteins. An increase in factor levels was observed after the thirty-fourth week of intrauterine life for most of the coagulation activators and inhibitors, but only factors V and VIII reached adult values at birth. This study therefore showed that fetal hemostasis is a dynamic system that evolves gradually toward the neonatal state and then toward the adult state.

摘要

对285例孕19至38周的健康胎儿的凝血蛋白进行了测定,并与60例正常足月新生儿及40例成人对照组进行比较。在整个宫内生活期间,胎儿凝血筛查试验(凝血酶原时间、活化部分凝血活酶时间和凝血酶凝结时间)延长是由维生素K依赖因子(II、VII、IX和X)、接触因子(XI、XII、前激肽释放酶和高分子量激肽原)、因子V、因子VIII和纤维蛋白原水平较低所致。还发现抗凝血酶III、肝素辅因子II、蛋白C和蛋白S以及组织因子途径抑制物水平较低,这些可能有助于维持令人满意的止血平衡。通过免疫测定和功能测定对其中一些参数进行了评估,以检测可能的 “胎儿” 蛋白。对于大多数凝血激活剂和抑制剂,在宫内生活第34周后观察到因子水平升高,但只有因子V和VIII在出生时达到成人水平。因此,本研究表明胎儿止血是一个动态系统,它逐渐向新生儿状态演变,然后向成人状态演变。

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