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胎儿及新生儿溶血病中母亲、胎儿和新生儿的实验室监测

Laboratory Monitoring of Mother, Fetus, and Newborn in Hemolytic Disease of Fetus and Newborn.

作者信息

Dziegiel Morten Hanefeld, Krog Grethe Risum, Hansen Anne Todsen, Olsen Marianne, Lausen Birgitte, Nørgaard Lone Nikoline, Bergholt Thomas, Rieneck Klaus, Clausen Frederik Banch

机构信息

Department of Clinical Immunology, Copenhagen University Hospital, Rigshospitalet, Copenhagen, Denmark.

Department of Clinical Medicine, University of Copenhagen, Copenhagen, Denmark.

出版信息

Transfus Med Hemother. 2021 Sep 8;48(5):306-315. doi: 10.1159/000518782. eCollection 2021 Oct.

Abstract

BACKGROUND

Laboratory monitoring of mother, fetus, and newborn in hemolytic disease of fetus and newborn (HDFN) aims to guide clinicians and the immunized women to focus on the most serious problems of alloimmunization and thus minimize the consequences of HDFN in general and of anti-D in particular. Here, we present the current approach of laboratory screening and testing for prevention and monitoring of HDFN at the Copenhagen University Hospital in Denmark.

SUMMARY

All pregnant women are typed and screened in the 1st trimester. This serves to identify the RhD-negative pregnant women who at gestational age (GA) of 25 weeks are offered a second screen test and a non-invasive fetal RhD prediction. At GA 29 weeks, and again after delivery, non-immunized RhD-negative women carrying an RhD-positive fetus are offered Rh immunoglobulin. If the 1st trimester screen reveals an alloantibody, antenatal investigation is initiated. This also includes RhD-positive women with alloantibodies. Specificity and titer are determined, the fetal phenotype is predicted by non-invasive genotyping based on cell-free DNA (RhD, K, Rhc, RhC, RhE, ABO), and serial monitoring of titer commences. Based on titers and specificity, monitoring with serial peak systolic velocity measurements in the fetal middle cerebral artery to detect anemia will take place. Intrauterine transfusion is given when fetal anemia is suspected. Monitoring of the newborn by titer and survival of fetal red blood cells by flow cytometry will help predict the length of the recovery of the newborn.

摘要

背景

对胎儿和新生儿溶血病(HDFN)中的母亲、胎儿及新生儿进行实验室监测,旨在引导临床医生和免疫女性关注同种免疫最严重的问题,从而总体上尽量减少HDFN的后果,尤其是抗-D的后果。在此,我们介绍丹麦哥本哈根大学医院预防和监测HDFN的实验室筛查及检测的当前方法。

总结

所有孕妇在孕早期进行血型鉴定和筛查。这有助于识别出RhD阴性孕妇,在孕25周时为她们提供第二次筛查试验和无创胎儿RhD预测。在孕29周时,以及分娩后,再次为怀有RhD阳性胎儿的未免疫RhD阴性女性提供Rh免疫球蛋白。如果孕早期筛查发现同种抗体,则启动产前检查。这也包括有同种抗体的RhD阳性女性。确定特异性和效价,通过基于游离DNA(RhD、K、Rhc、RhC、RhE、ABO)的无创基因分型预测胎儿表型,并开始对效价进行连续监测。根据效价和特异性,通过连续测量胎儿大脑中动脉的收缩期峰值流速来监测以检测贫血。当怀疑胎儿贫血时进行宫内输血。通过效价监测新生儿,并通过流式细胞术监测胎儿红细胞的存活情况,这将有助于预测新生儿恢复的时长。

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