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预防Rh血型免疫及治疗受损胎儿。

Prevention of Rh isoimmunization and treatment of the compromised fetus.

作者信息

Grannum P A, Copel J A

机构信息

Department of Obstetrics and Gynecology, Yale University School of Medicine, New Haven, CT 06510.

出版信息

Semin Perinatol. 1988 Oct;12(4):324-35.

PMID:3146812
Abstract

Intrauterine intravascular transfusion for the treatment of severe erythroblastosis fetalis has resulted in a number of benefits: (a) Direct access to the fetal vasculature allows an accurate assessment and prompt correction of anemia, albeit temporary. In contrast, intraperitoneally transfused blood may be absorbed erratically, especially in the face of ascites. (b) Intravascular treatments can be performed, in general, as early as 17 weeks of gestation, earlier than intraperitoneal approaches permit. (c) Reversal of hydrops along with the correction of anemia and hypoproteinemia has significantly reduced neonatal morbidity and mortality. None of the surviving neonates in our series required either thoracentesis or paracentesis following delivery, and 40% did not require neonatal exchange transfusion. (d) Treatments may be safely performed until pulmonic maturity has been established and/or an EFW of greater than 2,000 g has been reached, reducing problems of prematurity. (e) Central vein and umbilical vein hypertension may be arrested or prevented, thereby allowing fetal liver function to return to normal. While isoimmunization stands as a disease that has been quite successfully reduced in frequency and severity by the careful attention and treatment by obstetricians, cases still occur. Due to the reduced frequency of severe disease, fewer physicians are trained and experienced in performing this difficult procedure. As fewer transfusions are required, the value of regionalized treatment centers will have to be considered carefully, in order to maximize the experience and efficiency of the intravascular intrauterine transfusion treatment teams.

摘要

宫内血管内输血治疗严重胎儿红细胞增多症带来了诸多益处

(a) 直接进入胎儿血管系统能够准确评估并迅速纠正贫血,尽管只是暂时的。相比之下,经腹腔输注的血液吸收情况不稳定,尤其是在有腹水的情况下。(b) 一般而言,血管内治疗最早可在妊娠17周时进行,比腹腔内治疗允许的时间更早。(c) 水肿的消退以及贫血和低蛋白血症的纠正显著降低了新生儿发病率和死亡率。在我们的系列病例中,存活的新生儿在出生后均无需进行胸腔穿刺或腹腔穿刺,40%的新生儿也无需进行新生儿换血治疗。(d) 治疗可安全进行,直至肺成熟或胎儿估计体重超过2000克,从而减少了早产问题。(e) 中心静脉和脐静脉高压可能得到控制或预防,进而使胎儿肝功能恢复正常。虽然通过产科医生的悉心关注和治疗,血型同种免疫疾病的发生率和严重程度已大幅降低,但病例仍有发生。由于严重疾病的发生率降低,接受过这种困难操作培训且有经验的医生越来越少。由于所需输血次数减少,必须仔细考虑区域化治疗中心的价值,以最大限度地提高血管内宫内输血治疗团队的经验和效率。

相似文献

1
Prevention of Rh isoimmunization and treatment of the compromised fetus.预防Rh血型免疫及治疗受损胎儿。
Semin Perinatol. 1988 Oct;12(4):324-35.
2
[Usefulness of intraperitoneal transfusion under direct ultrasound guidance].[直接超声引导下腹腔内输血的效用]
Ginecol Obstet Mex. 1991 Apr;59:128-33.
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[Analysis and perinatal outcome after intravascular transfusion].[血管内输血后的分析及围产期结局]
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Percutaneous umbilical transfusion in severe rhesus isoimmunization: resolution of fetal hydrops.严重恒河猴血型不合溶血病的经皮脐血输血:胎儿水肿的消退
Am J Obstet Gynecol. 1987 Dec;157(6):1369-75. doi: 10.1016/s0002-9378(87)80226-0.
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Maternal ABO-mismatched blood for intrauterine transfusion of severe hemolytic disease of the newborn due to anti-Rh17.用于因抗Rh17导致的新生儿严重溶血病宫内输血的母亲ABO血型不匹配血液。
Transfusion. 2004 Sep;44(9):1357-60. doi: 10.1111/j.1537-2995.2004.04082.x.
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[Intrauterine transfusión in alloimmunization Rh in México 1987-2008].[1987 - 2008年墨西哥Rh血型同种免疫中的宫内输血]
Ginecol Obstet Mex. 2010 Sep;78(9):469-77.
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Intravascular intrauterine transfusion for severe erythroblastosis fetalis using different techniques.
Fetal Ther. 1988;3(1-2):50-9. doi: 10.1159/000263334.
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In-utero intravascular transfusion of the fetus for the management of severe Rhesus isoimmunization--a reappraisal.宫内血管内输血治疗严重恒河猴血型不合免疫反应——重新评估
Br J Obstet Gynaecol. 1987 Nov;94(11):1068-73. doi: 10.1111/j.1471-0528.1987.tb02291.x.
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[Maternal blood intrauterine transfusions in the therapy of red-cell alloimmunization performed in three difficult cases].[三例疑难病例中红细胞同种免疫治疗的母血宫内输血]
Ginekol Pol. 2014 Sep;85(9):703-7.
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Fetal transfusion.胎儿输血
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