Klüter H, Bubel S, Kirchner H, Wilhelm D
Institute of Immunology and Transfusion Medicine, University of Lübeck School of Medicine, Germany.
Transfusion. 1999 Nov-Dec;39(11-12):1179-84. doi: 10.1046/j.1537-2995.1999.39111179.x.
Nonhemolytic transfusion reactions (NHTRs) frequently occur after platelet transfusions. White cell (WBC)-derived inflammatory cytokines can cause these reactions, but they are rarely found in WBC-poor platelet preparations. Transfusion reactions were investigated with regard to the residual WBC content in the stored platelet concentrate in two consecutive study periods.
In the first study period, platelet concentrates were WBC-reduced by bedside filtration. In the second period, all platelet concentrates were filtered before storage. Recipients who experienced transfusion reactions were examined with regard to their main clinical symptoms during and after transfusion. In the supernatant of the involved platelet concentrates, concentrations of interleukin (IL)-1beta, IL-6, IL-8, tumor necrosis factor (TNF)alpha, macrophage inflammatory protein 1alpha, and RANTES were analyzed.
The incidence of transfusion reactions remained steady when the transfusion regimen was changed from bedside filtration to prestorage WBC filtration (1.63% and 1.56%; p = 0.84). In both periods, NHTRs were predominantly of allergic origin. Inflammatory mediators IL-1beta, IL-6, IL-8, and TNFalpha were detectable in only a minority of platelet components involved in NHTRs. Platelet concentrates involved in allergic reactions contained high concentrations of RANTES (668 +/- 223 ng/mL).
Prestorage WBC filtration did not reduce the incidence of these reactions, and inflammatory cytokines were of minor relevance. The proinflammatory platelet-derived chemokine RANTES, which accumulates even in WBC-reduced platelet concentrates, was associated with allergic transfusion reactions. Platelet-derived mediators may be a key to understanding NHTRs.
非溶血性输血反应(NHTRs)在血小板输注后频繁发生。白细胞(WBC)衍生的炎性细胞因子可引发这些反应,但在白细胞含量低的血小板制剂中很少发现。在两个连续的研究阶段中,针对储存的血小板浓缩物中的残留白细胞含量对输血反应进行了调查。
在第一个研究阶段,通过床边过滤对血小板浓缩物进行白细胞去除。在第二个阶段,所有血小板浓缩物在储存前进行过滤。对发生输血反应的受血者在输血期间及输血后的主要临床症状进行检查。对相关血小板浓缩物的上清液中白细胞介素(IL)-1β、IL-6、IL-8、肿瘤坏死因子(TNF)α、巨噬细胞炎性蛋白1α和调节激活正常T细胞表达和分泌的趋化因子(RANTES)的浓度进行分析。
当输血方案从床边过滤改为储存前白细胞过滤时,输血反应的发生率保持稳定(分别为1.63%和1.56%;p = 0.84)。在两个阶段中,NHTRs主要为过敏源性。炎性介质IL-1β、IL-6、IL-8和TNFα仅在少数参与NHTRs的血小板成分中可检测到。参与过敏反应的血小板浓缩物中含有高浓度的RANTES(668±223 ng/mL)。
储存前白细胞过滤并未降低这些反应的发生率,炎性细胞因子的相关性较小。即使在白细胞减少的血小板浓缩物中也会积累的促炎性血小板衍生趋化因子RANTES与过敏性输血反应相关。血小板衍生介质可能是理解NHTRs的关键。
