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同种免疫性血小板减少症的管理:产前诊断及宫内输注母体血小板

Management of alloimmune thrombocytopenia: antenatal diagnosis and in utero transfusion of maternal platelets.

作者信息

Kaplan C, Daffos F, Forestier F, Cox W L, Lyon-Caen D, Dupuy-Montbrun M C, Salmon C

机构信息

Service d'Immunologie Leuco-Plaquettaire, INTS, Paris, France.

出版信息

Blood. 1988 Jul;72(1):340-3.

PMID:3390610
Abstract

Neonatal alloimmune thrombocytopenia (NAIT) can cause severe bleeding in the central nervous system (CNS) and death or severe neurologic sequelae. The expression of the PLA1 antigen is detectable as early as 19 weeks of gestation. Alloimmunization can therefore lead to fetal thrombocytopenia very early in pregnancy. Until recently, we have had no means of detecting and assessing the severity of fetal thrombocytopenia during pregnancy. The level of the maternal antibody is not of a predictable value since 20% of the mothers had no circulating antibodies in our series. An alternative approach is to carry out investigations on fetal blood samplings. This management leads to an exact knowledge of the fetal status and antenatal diagnosis is feasible as early as the 21st week of gestation. Early diagnosis facilitates appropriate management and makes possible such therapeutic options as in utero maternal platelet transfusions. We report our experience in the antenatal diagnosis and management of nine cases with in utero transfusion in the six cases with severe thrombocytopenia. All neonates did well, with no signs of bleeding at birth. No side effects of therapy were noted after a period ranging from 6 months to 3 years.

摘要

新生儿同种免疫性血小板减少症(NAIT)可导致中枢神经系统(CNS)严重出血以及死亡或严重神经后遗症。PLA1抗原的表达早在妊娠19周时就可检测到。因此,同种免疫可在妊娠早期就导致胎儿血小板减少。直到最近,我们还没有办法在孕期检测和评估胎儿血小板减少的严重程度。由于在我们的系列研究中20%的母亲没有循环抗体,所以母体抗体水平没有可预测价值。另一种方法是对胎儿采血进行检查。这种处理方式能让我们确切了解胎儿状况,早在妊娠21周时就可行产前诊断。早期诊断有助于进行恰当处理,并使诸如宫内母体血小板输注等治疗选择成为可能。我们报告了9例产前诊断及管理的经验,其中6例严重血小板减少症患者接受了宫内输血。所有新生儿情况良好,出生时无出血迹象。在6个月至3年的观察期后,未发现治疗有副作用。

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