首页> 外文期刊>Transfusion: The Journal of the American Association of Blood Banks >Predicting the effect of transfusing only phenotype-matched RBCs to patients with sickle cell disease: theoretical and practical implications.
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Predicting the effect of transfusing only phenotype-matched RBCs to patients with sickle cell disease: theoretical and practical implications.

机译:预测仅将表型匹配的红细胞输注到镰状细胞疾病患者的效果:理论和实践意义。

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BACKGROUND: Transfusing only phenotype-matched RBCs has been recommended to reduce the incidence of alloimmunization to blood group antigens in patients with sickle cell disease (SCD). STUDY DESIGN AND METHODS: The expected benefit of phenotype matching was determined by identifying which of the existing blood group alloantibodies in patients with SCD who received conventional transfusions would not have been formed if they had received only phenotype-matched RBCs. By use of each patient's alloantibodies as a baseline, it was possible to identify specific alloantibodies that would not have been formed if each of five different phenotype-matching protocols had been used. RESULTS: During a 12-year period, 351 patients received transfusions with 8939 units of ABO- and D-matched RBCs. Of these, 102 patients (29.1%) formed at least one blood group alloantibody. An additional 35 patients with SCD with alloantibodies were identified by reviewing clinical records, yielding a total of 137 alloimmunized patients for inclusion in this study. If all transfusions had been selected by limited phenotype matching (C, c, E, e, and K, as well as for ABO and D), all alloantibodies would have been prevented for more than half (53.3%) of the 137 alloimmunized patients. If all transfusions had been matched for C, c, E, e, K, S, Fya, and Jkb, all antibodies would have been prevented for 70.8 percent of the 137 alloimmunized patients. Approximately 13.6 percent of random white blood donors would be expected to match a limited phenotype-matching protocol, whereas only 0.6 percent would match an extended phenotype-matching protocol. CONCLUSION: Limited phenotype matching would have prevented all alloantibodies in 53.3 percent of the patients who formed alloantibodies. This protocol requires RBCs that are readily available. Extended phenotype matching would have prevented alloimmunization in 70.8 percent of patients who formed alloantibodies. However, this would require phenotypes that are 22.7 times less prevalent among random blood donors and is therefore impractical for a long-term strategy.
机译:背景:已建议仅输注与表型匹配的红细胞,以减少镰状细胞病(SCD)患者对血型抗原的同种免疫的发生率。研究设计和方法:通过确定接受常规输血的SCD患者中哪些血型同种抗体如果仅接受与表型匹配的RBC不会形成,就可以确定表型匹配的预期益处。通过使用每个患者的同种异体抗体作为基准,可以鉴定出如果使用了五个不同表型匹配方案中的每一个都不会形成的特定同种异体抗体。结果:在12年期间,有351例患者接受了8939单位ABO和D匹配的RBC输血。其中102名患者(29.1%)形成了至少一种血型同种抗体。通过回顾临床记录,鉴定出另外35名SCD的同种抗体患者,总共137名接受同种免疫的患者纳入本研究。如果通过有限的表型匹配(C,c,E,e和K以及ABO和D)选择了所有输血,则在137个接受同种免疫的患者中,一半以上(53.3%)的同种抗体可以被预防。如果所有输血都匹配了C,c,E,e,K,S,Fya和Jkb,则在137名同种免疫患者中,所有抗体将被预防70.8%。预计约有13.6%的随机白血供者匹配有限的表型匹配方案,而只有0.6%的人将匹配扩展的表型匹配方案。结论:有限的表型匹配将阻止53.3%的形成同种抗体的患者出现所有同种抗体。该协议要求RBC随时可用。扩展的表型匹配将阻止形成同种抗体的患者中70.8%的同种免疫。但是,这将要求表型在随机献血者中的流行率降低22.7倍,因此对于长期策略而言是不切实际的。

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