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Epidemiology and management of fetal and neonatal alloimmune thrombocytopenia

机译:流行病学与胎儿和新生儿同种疫血小板减少症

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摘要

Fetal and neonatal alloimmune thrombocytopenia (FNAIT) is a disease in pregnancy characterized by maternal alloantibodies directed against the human platelet antigen (HPA). These antibodies can cause intracranial hemorrhage (ICH) or other major bleeding resulting in lifelong handicaps or death. Optimal fetal care can be provided by timely identification of pregnancies at risk. However, this can only be done by routinely antenatal screening. Whether nationwide screening is cost-effective is still being debated. HPA-1a alloantibodies are estimated to be found in 1 in 400 pregnancies resulting in severe burden and fetal ICH in 1 in 10.000 pregnancies. Antenatal treatment is focused on the prevention of fetal ICH and consists of weekly maternal IVIg administration. In high-risk FNAIT treatment should be initiated at 12-18 weeks gestational age using high dosage and in standard-risk FNAIT at 20-28 weeks gestational age using a lower dosage. Postnatal prophylactic platelet transfusions are often given in case of severe thrombocytopenia to prevent bleedings. The optimal threshold and product for postnatal transfusion is not known and international consensus is lacking. In this review practical guidelines for antenatal and postnatal management are offered to clinicians that face the challenge of reducing the risk of bleeding in fetuses and infants affected by FNAIT.
机译:胎儿和新生儿同种血管血小板减少症(FNAIT)是妊娠的疾病,其特征在于针对人血小板抗原(HPA)的母体丙胶质。这些抗体可引起颅内出血(ICH)或其他主要出血,导致终身障碍或死亡。可以通过及时鉴定风险的怀孕来提供最佳胎儿护理。但是,这只能通过常规的产前筛查来完成。全国范围内的筛查是否具有成本效益仍在争论。据估计,HPA-1A Alloantibodies在400人怀孕中发现,导致10.000人怀孕中的1个妊娠和胎儿胎儿。产前治疗的重点是预防胎儿,由每周母体IVIG管理组成。在高风险的Fnait治疗中,应在12-18周使用高剂量和标准风险Fnait在20-28周使用较低剂量的妊娠期妊娠期前期开始。在严重的血小板减少症以防止出血的情况下通常给出产后预防性血小板输血。出生后输血的最佳阈值和产品未知,缺乏国际共识。在这篇审查中,向临床医生提供了临床医生的实际指南,这些临床医生会面临减少受FNAIT影响的胎儿和婴儿出血风险的挑战。

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