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Thrombophilia risk is not increased in children after perinatal stroke

机译:围困后,血栓性风险不会增加儿童

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摘要

Perinatal stroke causes cerebral palsy and lifelong disability. Specific diseases are definable, but mechanisms are poorly understood. Evidence suggests possible associations between arterial perinatal stroke and prothrombotic disorders, but population-based, controlled, disease-specific studies are limited. Understanding thrombophilia in perinatal stroke informs pathogenesis modelsand clinicalmanagement. We conducted a population-based, prospective, case-control study to determine the association of specific perinatal stroke diseases with known thrombophilias. Children with idiopathic magnetic resonance imaging-classified neonatal arterial ischemic stroke (NAIS), arterial presumed perinatal ischemic stroke (APPIS), or fetal periventricular venous infarction (PVI) were recruited. Standardized thrombophilia evaluations were performed after 12 months of age on stroke cases and controls, including quantified proteins C and S, antithrombin, factors VIII/IX/XI, fibrinogen, lipoprotein(a), homocysteine, lupus anticoagulant, anticardiolipin antibodies and genotyping of factor V Leiden (FVL), factor II G20210A (FII), and methylenetetrahydrofolate reductase C677T. A total of 212 children were studied: 46 with NAIS, 34 with APPIS, 55 with PVI, and 77 controls (male, 53%; median age, 4.8 years). Of 14 parameters, no differences were observed in 12, including all common thrombophilias. Mean prothrombin time was shorter in arterial strokes (P < .001). Rates of antiphospholipid antibodies were low, comparable to those in controls, and resolved on repeat testing. FVL and FII rates were comparable to population norms. Total number of possible abnormalities did not differ between cases and controls. Our prospective, population-based, controlled, disease-specific study suggests minimal association between perinatal stroke and thrombophilia. This does not exclude the possibility of disordered coagulation at the time of stroke but suggests testing in childhood is not indicated.
机译:围产期中风引起脑瘫和终身残疾。具体疾病是可定义的,但机制明白很差。证据表明动脉围产手术和癌细胞紊乱之间可能的关联,但是基于人群的,受控,疾病特异性研究有限。了解围产期中风中的血栓形成通知发病机制和临床管理。我们进行了一项基于人群的,前瞻性的病例对照研究,以确定具有已知血栓性血栓性的特异性围产卒中疾病的关联。发作性磁共振成像的儿童分类为新生儿动脉缺血性卒中(NAIs),动脉推测围产期缺血性卒中(APPIS),或胎儿静脉静脉梗死(PVI)。在中风病例和对照组12个月后进行标准化血栓性评价,包括定量蛋白C和S,抗凝血酶,因子VIII / IX / XI,纤维蛋白原,脂蛋白(A),同纤维素,狼疮抗凝血剂,抗野生素抗体和因子基因分型V leiden(FVL),因子II G20210A(FII)和甲基四乙烯酸还原酶C677T。共有212名儿童研究:46例Nais,34例,Appis,55个,PVI和77个控制(男性,53%;中位年龄,4.8岁)。在14个参数中,在12中没有观察到差异,包括所有常见的血栓血管血管。平均凝血酶原时间在动脉卒中短(P <.001)。抗磷脂抗体的速率低,与对照组相当,并在重复测试上进行了解决。 FVL和FII率与人口规范相当。案例和控制之间的可能异常的总数并不不同。我们的前瞻性,基于人口,控制,疾病的疾病特异性研究表明围产期中风和血栓性血液干扰素之间的最小关系。这并不排除卒中时凝血无序凝血的可能性,但没有表明在儿童时期的测试。

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