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治疗性血浆置换和静脉注射免疫球蛋白作为孕期D同种免疫的主要治疗方法可避免进行宫内输血。

Therapeutic plasma exchange and intravenous immunoglobulin as primary therapy for D alloimmunization in pregnancy precludes the need for intrauterine transfusion.

作者信息

Bellone Michael, Boctor Fouad N

机构信息

Division of Transfusion Medicine, Department of Pathology, North Shore University Hospital and Hofstra North Shore-LIJ School of Medicine, Manhasset, New York.

出版信息

Transfusion. 2014 Aug;54(8):2118-21. doi: 10.1111/trf.12633. Epub 2014 Mar 28.

DOI:10.1111/trf.12633
PMID:24673470
Abstract

BACKGROUND

Maternal D alloimmunization detected in early gestation requires aggressive intervention to prevent severe fetal anemia. An intrauterine transfusion (IUT) is indicated to prevent fetal death once severe fetal anemia has been detected, but is not without risk. Protocols combining therapeutic plasma exchange (TPE) and intravenous immunoglobulin (IVIG) have been described, but they usually bridge to IUT.

STUDY DESIGN AND METHODS

We describe a 27-year-old G4, P0-1-2-0 Caucasian female with a history of ruptured ectopic pregnancy presented at 12 weeks' gestation with a very high anti-D titer (2048). TPE was performed on that week and twice more in the following week, with a fourth final exchange during Week 14. A loading dose of IVIG (2 g/kg) was administered over 2 days after the third TPE and then 1 g/kg per week until Week 28 (total, 14 doses).

RESULTS

The antibody titer decreased to 256 by the beginning of 15 weeks' gestation and remained stable at that level for the remainder of the pregnancy. Doppler ultrasonographic measurements of the fetal middle cerebral artery peak flow velocity performed throughout gestation showed no evidence of fetal anemia. A healthy male infant was delivered at 37 weeks' gestation with mild immune-mediated hemolysis. The infant underwent successful treatment with an IVIG dose of 750 mg/kg and a red blood cell exchange.

CONCLUSION

Our unique TPE-IVIG protocol was successful at preventing the onset of severe fetal anemia in a patient with high titer anti-D. Since IUT may be fatal, our approach offers a safer and less-invasive treatment regime that can adequately sustain a fetus until term.

摘要

背景

妊娠早期检测到母体D同种免疫需要积极干预以预防严重胎儿贫血。一旦检测到严重胎儿贫血,就需要进行宫内输血(IUT)以预防胎儿死亡,但并非没有风险。已经描述了将治疗性血浆置换(TPE)和静脉注射免疫球蛋白(IVIG)相结合的方案,但它们通常是过渡到IUT的桥梁。

研究设计与方法

我们描述了一名27岁、孕4产0-1-2-0的白人女性,有异位妊娠破裂史,孕12周时抗-D效价非常高(2048)。在那周进行了TPE,并在接下来的一周又进行了两次,在第14周进行了第四次也是最后一次置换。在第三次TPE后2天内给予负荷剂量的IVIG(2 g/kg),然后每周1 g/kg直至第28周(共14剂)。

结果

到孕15周开始时,抗体效价降至256,并在妊娠剩余时间保持在该水平稳定。整个孕期对胎儿大脑中动脉峰值流速进行的多普勒超声测量未显示胎儿贫血的迹象。一名健康男婴在孕37周出生,有轻度免疫介导的溶血。婴儿接受了750 mg/kg剂量的IVIG和红细胞置换治疗并成功治愈。

结论

我们独特的TPE-IVIG方案成功预防了一名高滴度抗-D患者严重胎儿贫血的发生情况。由于IUT可能是致命的,我们的方法提供了一种更安全、侵入性更小的治疗方案,可以使胎儿充分维持到足月。

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