Mangare Caroline, Mbugua Amos, Maturi Peter, Rajab Jamila, Blasczyk Rainer, Heuft Hans-Gert
Jomo Kenyatta University of Agriculture and Technology, Nairobi, Kenya.
Kenyatta National Hospital/University of Nairobi, Department of Hematology and Blood Transfusion, Nairobi, Kenya.
Afr J Lab Med. 2015 Sep 25;4(1):297. doi: 10.4102/ajlm.v4i1.297. eCollection 2015.
Currently, no data are available on the prevalence of red blood cell (RBC) antibody formation amongst Kenyan patients with multiple transfusion needs, such as patients with sickle cell disease (SCD) or haematological malignancies (HM) and solid (SM) malignancies.
We determined the prevalence and specificities of RBC alloantibodies and autoantibodies in two patient groups with recurrent transfusion demands at Kenyatta National Hospital, Nairobi, Kenya.
Between February and August 2014, 300 samples from SCD, HM and SM patients were collected and screened for alloantibodies. Samples from 51 healthy blood donors were screened for irregular antibodies and phenotyped.
Amongst the 228 patients with viable samples (SCD, = 137; HM, = 48; SM, = 43), the median transfusion frequency was two to three events per group, 38 (16.7%) were RBC immunised and 32 (14.0%) had a positive direct antiglobulin test. We identified specific alloantibodies in six patients (2.6%). Four of these six were SCD patients (2.9%) who had specific RBC alloantibodies (anti-C, anti-M, anti-Co, anti-S); amongst HM patients one had anti-K and one had anti-Le. RBC autoantibody prevalence was 3.1% (7/228). Amongst the healthy blood donors, the Rr, ccD.ee and Rr, ccD.Ee phenotypes accounted for 82% of the Rhesus phenotypes and all were Kell negative.
The numbers of transfusions and the rates of RBC alloantibodies are low and the most important RBC alloantibody-inducing blood group antigens are relatively homogeneously distributed in this population. A general change in the Kenyatta National Hospital pre-transfusion test regimen is thus not necessary. The current transfusion practice should be reconsidered if transfusion frequencies increase in the future.
目前,尚无关于肯尼亚有多次输血需求的患者(如镰状细胞病[SCD]患者、血液系统恶性肿瘤[HM]患者和实体恶性肿瘤[SM]患者)中红细胞(RBC)抗体形成发生率的数据。
我们确定了肯尼亚内罗毕肯雅塔国家医院两组有反复输血需求患者中RBC同种抗体和自身抗体的发生率及特异性。
2014年2月至8月期间,收集了300份来自SCD、HM和SM患者的样本并筛查同种抗体。对51名健康献血者的样本进行不规则抗体筛查和血型鉴定。
在228例有可用样本的患者中(SCD患者137例、HM患者48例、SM患者43例),每组的输血频率中位数为两到三次,38例(16.7%)患者红细胞免疫,32例(14.0%)患者直接抗球蛋白试验呈阳性。我们在6例患者(2.6%)中鉴定出特异性同种抗体。这6例患者中有4例为SCD患者(2.9%),他们有特异性RBC同种抗体(抗-C、抗-M、抗-Co、抗-S);在HM患者中,1例有抗-K,1例有抗-Le。RBC自身抗体发生率为3.1%(7/228)。在健康献血者中,Rr、ccD.ee和Rr、ccD.Ee表型占恒河猴血型表型的82%,且均为凯尔阴性。
输血次数和RBC同种抗体发生率较低,在该人群中最重要的诱导RBC同种抗体的血型抗原分布相对均匀。因此,肯雅塔国家医院目前的输血前检测方案无需进行总体改变。如果未来输血频率增加,则应重新考虑当前的输血实践。
