Transfusion support during childbirth for a woman with anti-U and the RHDweak D type 4.0* allele.

Q4 Medicine

Immunohematology Pub Date : 2021-03-01 DOI:10.21307/immunohematology-2021-001

Q Yin, K Srivastava, D G Brust, W A Flegel

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引用次数: 5

Abstract

D- red blood cells (RBCs), always in short supply, and Rh immune globulin (RhIG) are not needed for patient care if D+ RBCs can safely be transfused. According to a recent work group recommendation, patients with the RHD*weak D type 4.0 allele can be considered D+. We report an African American woman who presented for delivery at the end of the third trimester, at which time anti-U and a serologic weak D phenotype were recognized, requiring U-, D- RBC units. We obtained 3 U- RBC units, including 1 D- unit. Later, the RHD*weak D type 4.0 allele was determined by RHD genotyping, only 6 days before delivery. The patient had an uneventful vaginal delivery of a D+ baby. No transfusion was needed for mother or baby. In this case, a pregnant woman with the RHD*weak D type 4.0 allele can safely be managed as D+, relaxing the unnecessary D- restriction for the limited U- RBC supply. The procured U-, D- RBC unit was frozen with 14 days of shelf-life remaining. To conserve D- RBC units, not limited to U-, for patients with a definite need, we recommend molecular analysis of a serologic weak D phenotype before a transfusion becomes imminent. The best time to resolve a serologic weak D phenotype with RHD genotyping is early in a pregnancy. Immunohematology 2021;37:1-4 .

D– red blood cells (RBCs), always in short supply, and Rh immune globulin (RhIG) are not needed for patient care if D+ RBCs can safely be transfused. According to a recent work group recommendation, patients with the RHD*weak D type 4.0 allele can be considered D+. We report an African American woman who presented for delivery at the end of the third trimester, at which time anti-U and a serologic weak D phenotype were recognized, requiring U–, D– RBC units. We obtained 3 U– RBC units, including 1 D– unit. Later, the RHD*weak D type 4.0 allele was determined by RHD genotyping, only 6 days before delivery. The patient had an uneventful vaginal delivery of a D+ baby. No transfusion was needed for mother or baby. In this case, a pregnant woman with the RHD*weak D type 4.0 allele can safely be managed as D+, relaxing the unnecessary D– restriction for the limited U– RBC supply. The procured U–, D– RBC unit was frozen with 14 days of shelf-life remaining. To conserve D– RBC units, not limited to U–, for patients with a definite need, we recommend molecular analysis of a serologic weak D phenotype before a transfusion becomes imminent. The best time to resolve a serologic weak D phenotype with RHD genotyping is early in a pregnancy. Immunohematology 2021;37:1–4 .

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携带抗u和RHD*弱D型4.0等位基因的妇女分娩时的输血支持。

如果D+红细胞可以安全地输注，总是供不应求的D-红细胞(rbc)和Rh免疫球蛋白(rhg)就不需要用于患者护理。根据最近的一项工作组建议，携带RHD*弱D型4.0等位基因的患者可被视为D+。我们报告了一位非裔美国妇女，她在妊娠晚期准备分娩，当时发现了抗U和血清学弱D表型，需要U-， D- RBC单位。我们获得了3个U- RBC单位，包括1个D-单位。随后，仅在分娩前6天，通过RHD基因分型检测RHD*弱D型4.0等位基因。该患者顺利阴道分娩了一名D+婴儿。母亲和婴儿都不需要输血。在这种情况下，携带RHD*弱D型4.0等位基因的孕妇可以被安全地管理为D+，因为有限的U- RBC供应放松了不必要的D-限制。将获得的U-， D- RBC单位冷冻，保存期限为14天。为了保存D-红细胞单位，不限于U-，对于有明确需要的患者，我们建议在输血迫在眉睫之前进行血清学弱D表型的分子分析。用RHD基因分型解决血清学弱D表型的最佳时间是在妊娠早期。免疫血液学2021;37:1-4 .D -红细胞(rbc)总是供不应求，如果D+红细胞可以安全输注，则患者护理不需要Rh免疫球蛋白(rhg)。根据最近的一项工作组建议，携带RHD*弱D型4.0等位基因的患者可被视为D+。我们报告了一位非裔美国妇女，她在妊娠晚期准备分娩，当时发现了抗U和血清学弱D表型，需要U -， D - RBC单位。我们获得了3个U - RBC单位，包括1个D -单位。随后，仅在分娩前6天，通过RHD基因分型检测RHD*弱D型4.0等位基因。该患者顺利阴道分娩了一名D+婴儿。母亲和婴儿都不需要输血。在这种情况下，携带RHD*弱D型4.0等位基因的孕妇可以被安全地管理为D+，因为有限的U - RBC供应放松了不必要的D -限制。将获得的U -， D - RBC单位冷冻，保存期限为14天。为了保存D -红细胞单位，不限于U -，对于有明确需要的患者，我们建议在输血迫在眉睫之前进行血清学弱D表型的分子分析。用RHD基因分型解决血清学弱D表型的最佳时间是在妊娠早期。免疫血液学2021;37:1-4。

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来源期刊

Immunohematology Medicine-Medicine (all)

CiteScore

1.30

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0.00%

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