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一项旨在降低与严重新生儿同种免疫性血小板减少症相关的死亡率和严重发病率的筛查与干预计划。

A screening and intervention program aimed to reduce mortality and serious morbidity associated with severe neonatal alloimmune thrombocytopenia.

作者信息

Kjeldsen-Kragh Jens, Killie Mette Kjaer, Tomter Geir, Golebiowska Elzbieta, Randen Ingrid, Hauge Reidun, Aune Berit, Øian Pål, Dahl Lauritz B, Pirhonen Jouko, Lindeman Rolf, Husby Henrik, Haugen Guttorm, Grønn Morten, Skogen Bjørn, Husebekk Anne

机构信息

Department of Immunity, Ullevål University Hospital, 0407 Oslo, Norway.

出版信息

Blood. 2007 Aug 1;110(3):833-9. doi: 10.1182/blood-2006-08-040121. Epub 2007 Apr 11.

DOI:10.1182/blood-2006-08-040121
PMID:17429009
Abstract

The study's objective was to identify HPA 1a-negative women and to offer them an intervention program aimed to reduce morbidity and mortality of neonatal alloimmune thrombocytopenia (NAIT). HPA 1 typing was performed in 100 448 pregnant women. The HPA 1a-negative women were screened for anti-HPA 1a. In immunized women, delivery was performed by Cesarean section 2 to 4 weeks prior to term, with platelets from HPA 1a-negative donors reserved for immediate transfusion if petechiae were present and/or if platelet count was less than 35 x 10(9)/L. Of the women screened, 2.1% were HPA 1a negative, and anti-HPA 1a was detected in 10.6% of these. One hundred seventy pregnancies were managed according to the intervention program, resulting in 161 HPA 1a-positive children. Of these, 55 had severe thrombocytopenia (< 50 x 10(9)/L), including 2 with intracranial hemorrhage (ICH). One woman with a twin pregnancy missed the follow-up and had one stillborn and one severely thrombocytopenic live child. In 15 previous prospective studies (136 814 women) there were 51 cases of severe NAIT (3 intrauterine deaths and 7 with ICH). Acknowledging the limitation of comparing with historic controls, implementation of our screening and intervention program seemed to reduce the number of cases of severe NAIT-related complications from 10 of 51 to 3 of 57.

摘要

该研究的目的是识别HPA 1a阴性女性,并为她们提供一项旨在降低新生儿同种免疫性血小板减少症(NAIT)发病率和死亡率的干预计划。对100448名孕妇进行了HPA 1分型。对HPA 1a阴性女性进行抗HPA 1a筛查。对于已免疫的女性,在预产期前2至4周进行剖宫产,如果出现瘀点和/或血小板计数低于35×10⁹/L,则保留来自HPA 1a阴性供者的血小板以备立即输血。在接受筛查的女性中,2.1%为HPA 1a阴性,其中10.6%检测到抗HPA 1a。170例妊娠按照干预计划进行管理,共娩出161名HPA 1a阳性儿童。其中,55例有严重血小板减少症(<50×10⁹/L),包括2例颅内出血(ICH)。一名怀有双胞胎的女性错过随访,产下一名死胎和一名严重血小板减少症活婴。在之前的15项前瞻性研究(136814名女性)中,有51例严重NAIT(3例宫内死亡和7例ICH)。尽管认识到与历史对照比较存在局限性,但我们的筛查和干预计划的实施似乎将严重NAIT相关并发症的病例数从51例中的10例减少至57例中的3例。

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