反复输血地中海贫血儿童血清免疫球蛋白水平变化及其与迟发性溶血性输血反应的相关性研究

目的 探讨反复输血地中海贫血儿童血清免疫球蛋白水平变化及其与迟发性溶血性输血反应(delayed hemolytic transfusion reactions, DHTR)的相关性。方法 收集2022年6月-2023年4月期间到本院接受输血治疗的地中海贫血儿童(观察组)及健康体检儿童(对照组)血清标本,运用流式细胞仪CBA多因子定量检测技术,检测血清免疫球蛋白(IgG亚类、IgM、IgA、IgE、IgD)水平,比较2组儿童血清免疫球蛋白差异;按照不同输血次数分为4组:≤10次、11~30次、31~50次、>50次,各组采用单因素方差分析比较不同输血次数与血清免疫球蛋白水平之间的差异;将DHTR的地中海贫血儿童分为溶血组,未发生DHTR的地中海贫血儿童分为非溶血组,比较2组儿童血清免疫球蛋白(IgG亚类、IgM、IgA、IgE、IgD)之间的变化,探讨反复输血的地中海贫血儿童血清免疫球蛋白与DHTR的相关性。结果 血清免疫球蛋白IgG1、IgG3、IgG4、IgA观察组明显高于对照组,分别增加了(2.07±2.12)、(0.67±2.03)、(0.30±0.37)、(6.04±11.40)mg/mL,IgD观察组明显低于对照组,降低了(0.03±0.01)mg/mL,P<0.05;IgG2、IgM、IgE 2组之间,P>0.05。输血次数与血清免疫球蛋白之间的相关性:随着输血次数增加,IgG1、IgG4均明显增高,4组IgG1依次增加(0.30±0.62)、(0.41±0.51)、(3.60±3.48)mg/mL,IgG4依次增加(0.12±0.13)、(0.22±0.07)、(0.21±0.38)mg/mL,IgG2、IgM、IgD明显降低,4组IgG2、IgM、IgD依次降低(0.91±1.50)、(0.14±0.10)、(0.05±0.05)mg/mL,与输血次数之间有显著差异性,P<0.05;IgG3、IgA、IgE与输血次数之间无显著差异性,P>0.05。IgG1、IgG3、IgG4溶血组明显高于非溶血组,分别增加了:IgG1(4.44±3.41),IgG3(0.73±1.26),IgG4(0.52±0.40)mg/mL,IgD溶血组明显低于非溶血组,降低了(0.00±0.06)mg/mL,P<0.05;IgG2、IgM、IgA、IgE溶血组与非溶血组之间,P>0.05。结论 反复输血的地中海贫血儿童血清免疫球蛋白水平异常;反复输血的地中海贫血儿童不同输血次数与血清免疫球蛋白之间存在相关差异性;反复输血的地中海贫血儿童发生DHTR的相关血清免疫球蛋白为IgG1、IgG3、IgG4。

抗-M、抗-Jk^(a)序贯产生致2次迟发性溶血性输血反应及应对策略

目的 通过追踪1例因输血后回忆反应连续产生意外抗体导致迟发性溶血性输血反应的患者,探讨有输血史、妊娠史患者群体的输血管理措施及应对策略。方法 对1例连续发生迟发性溶血反应患者进行ABO、Rh、MN及Kidd血型鉴定、直接抗人球蛋白试验、意外抗体筛查及抗体鉴定,鉴定后用相应红细胞检测其抗体效价,同时筛选合适的红细胞供患者后续治疗使用。结果 患者血型为B型RhD(+)、CCDee,第1次输血前抗筛阴性,交叉配血相合,输血后d8患者血红蛋白降至57 g/L,抗筛阳性,抗体鉴定结果为抗-M,患者输入的血液表型为M+N+,实验室结果表明患者发生了迟发性溶血。患者在输入M抗原阴性血液后,实验室检查结果仍提示有迟发性血清学输血反应发生,抗体鉴定显示患者产生了新的抗-Jka,而输入的红细胞表型为M-N+、Jk(a+b-)。此后选择B型、RhD(+)、M-N+、Jk(a-b+)的红细胞输注有效。结论 患者输血后初次检测出的同种抗体大多数会在几年内消失,当患者再次输血,则可能发生迟发性溶血反应,为已产生同种抗体输血患者建立输血管理档案、制作卡片供患者保存,在下次需要输血时告知医生和输血科人员,可大大减少迟发性溶血性输血反应的发生。

溶血性输血反应病例分析及国内文献回顾

目的调查溶血性输血反应发生的原因,鉴别临床症状及严重程度,探索临床检测方法思路及意义,为安全合理用血提供依据。方法对本院发生溶血性输血反应的3个病例进行临床资料分析,复查血型,意外抗体筛查,血清及放散液抗体鉴定,同时对国内溶血性输血反应病例进行文献回顾。结果病例1诊断为迟发性溶血性输血反应,输血7d后抗体鉴定为抗-JK^(a);病例2诊断为急性溶血性输血反应,输血后d5和d7分别检出抗-Ce和抗-JK^(b);病例3诊断为不明类型的溶血性输血反应,输血3 d后检出抗-E。2005—2021年国内共报告33例溶血性输血反应,包括14例急性溶血性输血反应、18例迟发性溶血性输血反应,另1例未进行分类。回顾33例溶血反应原因,其中ABO血型系统抗体4例,Rh血型系统抗体17例,Kidd血型系统抗体4例,非免疫因素导致3例,未注明抗体特异性5例。结论多种血型系统抗体均可引起溶血反应。随着临床认识和实验室检测技术的提升,明确溶血原因,鉴定同种抗体类型,抗原同型输血,对用血安全有重要意义。

DEL RBC transfusion should be avoided in particular blood recipient in East Asia due to allosensitization and ineffectiveness

Previously, both primary and secondary anti-D alloimmunizations induced by "Asian type" DEL (RHD1227A allele) were observed in two incidents. We investigated how often these alloimmunization events occur. The transfusions of any D-negative patients were investigated in the First Affiliated Hospital of Xi'an Jiaotong University Medical College, China, during the entire 2009. The antigens of D, C, c, E, and e were routinely serotyped. The "Asian type" DEL variant was genotyped and the RHD heterozygote was determined through two published methods. The changes in anti-D levels were monitored by the indirect antiglobulin test (IAT) and flow cytometry. Thirty D-negative transfused patients were included in the study. We focused on 11 recipients who were transfused with packed red blood cells (RBCs) from DEL donors at least one time. Of those 11 recipients, seven were anti-D negative before transfusion and four were anti-D positive (one patient with an autoantibody). One of the seven pre-transfusion anti-D negative patients produced a primary-response anti-D after being transfused with 400 ml of DEL blood twice. All four pre-transfusion antibody positive patients were not observed hemoglobin (Hb) levels increased, as expected after transfusions. Two patients had an increase in anti-D from 1:8 to 1:64 by IAT, which was also shown by flow cytometry. None of the patients experienced an acute hemolytic episode. Our data indicated that the primary anti-D induced by DEL transfusion or the secondary anti-D elevated by DEL in a truly D-negative patient might not be unusual. We suggest that a truly D-negative childbearing-aged woman should avoid DEL transfusion to protect her from primary anti-D allosensitization. In addition, anti-D positive recipients should also avoid DEL red cell transfusion due to the delayed hemolytic transfusion reaction (DHTR).