Phenotyping of Rh and Kell blood group antigen in thalassemia and its impact on alloimmunization in a tertiary care hospital

IF 0.9 Q3 MEDICINE, GENERAL & INTERNAL Journal of Laboratory Physicians Pub Date : 2024-02-09 DOI:10.25259/jlp-2023-7-8-(1848)
Sonia Gupta, R. Kumar
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Abstract

Alloimmunization to red cell antigens is a dreaded complication in multitransfused patients, leading to difficulty in obtaining compatible red blood cell units and development of delayed hemolytic transfusion reactions. The objective of this study was to assess the impact of partial matched phenotype blood (for RhD, C, c, E, e, and Kell antigens) on alloimmunization in thalassemics versus non-phenotype matched blood (ABO & RhD). This cross-sectional study was conducted over a period of two years where 250 patients with thalassemias were enrolled. They were divided into two groups, patients in Group I (n = 180) who received partial matched phenotype blood since initiation of transfusion therapy and those in Group II (n = 70) subjects who received usual matched blood. All statistical calculations were done using statistical package for the social sciences (SPSS) 21 version. Data were described in terms of range, median (interquartile range [IQR]), frequencies, etc. The median (IQR) age of the study population was 12 (7–18) years (range 6 months–36 years). The most common Rh antibodies were anti-D (2.85%), anti-E (2.85%), anti-C (1.42%), and anti-c (1.42%), and Kell antibodies were (7.1%). It was seen that chances of developing autoantibodies (37% vs. 5%), alloantibodies 11 (15.7% vs. 0%), and transfusion reactions 25 (35.7% vs. 3.3%) were more in Group II subjects as compared to Group I. A significant difference was seen with febrile non-hemolytic transfusion reactions in between two groups 0.001 (95% confidence interval 2.98–65.73). Patients with thalassemia should be typed for RhD (C, c, E, and e) and Kell antigen before initiation of transfusion, which will help in reducing the rate of alloimmunization, autoimmunization, and frequency of transfusion and will improve the overall survival rate in thalassemia.
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地中海贫血症患者的 Rh 和 Kell 血型抗原表型及其对一家三级医院同种免疫的影响
红细胞抗原的同种免疫是多次输血患者的一种可怕的并发症,它导致患者难以获得相容的红细胞单位,并引发迟发性溶血性输血反应。这项研究旨在评估部分表型匹配血液(RhD、C、c、E、e 和 Kell 抗原)与非表型匹配血液(ABO 和 RhD)对地中海贫血症患者同种免疫的影响。他们被分为两组,第一组患者(n = 180)自输血治疗开始就接受部分表型匹配的血液,第二组患者(n = 70)接受通常匹配的血液。研究对象的年龄中位数(IQR)为 12(7-18)岁(6 个月-36 岁)。最常见的 Rh 抗体是抗-D(2.85%)、抗-E(2.85%)、抗-C(1.42%)和抗-C(1.42%),凯尔抗体为(7.1%)。与第一组相比,第二组受试者出现自身抗体(37% 对 5%)、异体抗体 11 例(15.7% 对 0%)和输血反应 25 例(35.7% 对 3.3%)的几率更高。001(95% 置信区间 2.98-65.73)。地中海贫血患者在开始输血前应进行 RhD(C、c、E 和 e)和 Kell 抗原分型,这将有助于降低同种免疫率、自身免疫率和输血频率,并提高地中海贫血患者的总体存活率。
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来源期刊
Journal of Laboratory Physicians
Journal of Laboratory Physicians MEDICINE, GENERAL & INTERNAL-
自引率
0.00%
发文量
99
审稿时长
31 weeks
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