Genotyped RHD+ red cells for D-positive patients with sickle cell disease with conventional RHD and unexpected anti-D

基因分型 Rh血型系统 医学 红细胞 基因型 输血 免疫学 等位基因 抗原 红细胞 抗体 内科学 基因 生物 遗传学
作者
Stella T. Chou,Julia Mewha,David F. Friedman,VIctoia Lazariu,Shaimaa Makrm,Gorka Ochoa,Sunitha Vege,Connie M. Westhoff
出处
期刊:Blood [Elsevier BV]
卷期号:144 (19): 2045-2049 被引量:1
标识
DOI:10.1182/blood.2024025602
摘要

Anti-D can occur in D-positive patients who inherit RHD genetic variants encoding partial D antigen expression, but unexpected anti-D is also found in the plasma of patients with sickle cell disease who have conventional RHD gene(s) and are transfused with units from Black donors. These anti-D are likely stimulated by variant Rh expressed on donor cells, however patients with anti-D, regardless of cause, are transfused for a lifetime with D-negative (Rh-negative) blood. This results in significant increased use of Rh-negative units, especially for those requiring chronic transfusion, which can strain Rh-negative blood inventories. We tested whether D-positive patients who made anti-D and had conventional RhD by RHD genotyping could safely be returned to D-positive transfusions without anti-D reappearance or compromised RBC survival using RHD genotype-matched units from Black donors. Five patients receiving chronic red cell exchange received an increasing number of D-positive units per procedure with a total of 72 D-positive RHD genotyped units transfused, with no anti-D restimulation. Unexpected anti-C and anti-E were identified during the study associated with donors with variant RHCE alleles. RH genotyping of D-positive units for transfusion may improve use and allocation of valuable Black donor units and reduce demand for Rh-negative blood.

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