胎儿红细胞增生症预防的最新进展综述。

IF 0.6 Q4 HEMATOLOGY
Asian Journal of Transfusion Science Pub Date : 2025-01-01 Epub Date: 2022-09-28 DOI:10.4103/ajts.ajts_50_22
Aishwarya Balasubramaniam, V Santhosh Kumar, S Priya
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引用次数: 0

摘要

胎儿红细胞增生症是印度新生儿和胎儿死亡的主要原因之一。这种疾病的特点是母体免疫球蛋白G抗体破坏新生儿或胎儿的红细胞,导致潜在的危及生命的后果。当rh阳性血型的母亲生下rh阴性血型的胎儿时,胎儿的红细胞会触发母体对rh抗原的抗体。抗- d抗体被激活作为这个过程的结果,这被称为等免疫。抗体反应的结果是,所有的红细胞被破坏,导致溶血、胆红素释放和贫血。血管内输血和腹腔内输血是产前治疗的例子,可以潜在地避免在妊娠早期对胎儿造成危险。光疗、交换补充输血和静脉注射免疫球蛋白是产后治疗(IVIG)的例子。IVIG疗法是强烈推荐的,因为它具有低风险的不良药物反应和广泛的存活率。为了避免等免疫,建议使用抗rh治疗。利用从母体血液中获得的无细胞胎儿DNA无创鉴定胎儿人血小板抗原1基因型是取得进展的一个例子。这种作为预防医学的研究仍处于早期阶段,血小板相当于Rho (D)人免疫球蛋白(RhoGAM)。胎儿红细胞增多症是高度可预防的,当它被诊断在其早期阶段。定期筛查所有ABO血型不相容的患者是必要的,以防止胎儿红母细胞病的风险。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

An overview of recent advances in the prevention of erythroblastosis fetalis.

An overview of recent advances in the prevention of erythroblastosis fetalis.

Erythroblastosis fetalis is one of the leading causes of death among newborns and fetuses in India. This condition is characterized by maternal immunoglobin G antibodies destroying the red blood cells (RBCs) of the neonate or fetus, resulting in potentially life-threatening consequences. When a mother with an Rh-positive blood group has a fetus with an Rh-negative blood group, the fetal RBCs trigger maternal antibodies against Rh-antigens. Anti-D antibodies are activated as a result of this process, which is known as isoimmunization. As a result of the antibody reaction, all of the erythrocytes are destroyed, resulting in hemolysis, bilirubin release, and anemia. Intravascular transfusions and intraperitoneal transfusions are examples of antenatal therapies that potentially avoid dangers to the fetus in the early stages of pregnancy. Phototherapy, exchange top-up transfusions, and intravenous immunoglobulin (IVIG) injections are examples of postnatal therapies (IVIG). IVIG therapy is highly recommended since it has a low risk of adverse medication responses and a wide range of survival rates. To avoid isoimmunization, anti-Rh D therapies are indicated. Noninvasive identification of the fetal human platelet antigen 1 genotype using cell-free fetal DNA obtained from maternal blood is one example of progress. This is still in the early stages of research as preventive medicine, the platelet equivalent of Rho (D) Immune Globulin Human (RhoGAM). The erythroblastosis fetalis is highly preventable when it is diagnosed at its early stages. Regular screening of all the patients with ABO incompatibility is necessary to prevent the risks of erythroblastosis fetalis.

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来源期刊
CiteScore
0.90
自引率
0.00%
发文量
56
审稿时长
44 weeks
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