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输注储存前过滤的血小板和红细胞后同种异体HLA和非HLA抗体的发生:一项前瞻性研究。

Occurrence of allogeneic HLA and non-HLA antibodies after transfusion of prestorage filtered platelets and red blood cells: a prospective study.

作者信息

Novotny V M, van Doorn R, Witvliet M D, Claas F H, Brand A

机构信息

Red Cross Blood Bank Leiden, The Netherlands.

出版信息

Blood. 1995 Apr 1;85(7):1736-41.

PMID:7703481
Abstract

The incidence and consequences of HLA and non-HLA immunization were evaluated in 229 patients with aplastic thrombocytopenia. All patients were transfused with prestorage filtered red blood cells and platelets. On admission, 29 patients presented with HLA antibodies due to prior immunization by pregnancy and/or blood transfusions. Of the 200 patients showing no detectable HLA antibodies on admission, 164 could be evaluated. HLA antibodies developed in 2.7% (3 of 112) of the patients with a negative risk history of prior immunization. The occurrence of HLA antibodies in patients with a history of previous pregnancies or prior non-leukocyte-depleted blood transfusions (risk history positive) was 31% (16 of 52). Of the total of 48 patients who were or became alloimmunized, 92% (44 of 48) had a positive risk history. Ten patients with broad multispecific HLA antibodies with a panel reactivity (PRA) of greater than 70% required transfusions with HLA-matched platelets. Patients with HLA antibodies with lower PRA could be supported by random donor platelets. Two patients developed platelet-specific antibodies, causing transfusion refractoriness that necessitated selecting platelets by the absence of a platelet-specific antigen. Using prestorage leukocyte depletion of red cells and platelets with less than 5 x 10(6) residual leukocytes, 95% of the patients, including patients with a previous risk history or with HLA antibodies with low PRA, can be supported with random donor transfusions for the entire duration of their thrombocytopenic periods.

摘要

对229例再生障碍性血小板减少症患者的HLA和非HLA免疫的发生率及后果进行了评估。所有患者均输注了预储存过滤的红细胞和血小板。入院时,29例患者因既往妊娠和/或输血免疫而出现HLA抗体。在入院时未检测到HLA抗体的200例患者中,164例可进行评估。既往免疫风险史阴性的患者中,2.7%(112例中的3例)产生了HLA抗体。既往有妊娠史或既往接受未去除白细胞输血(风险史阳性)的患者中,HLA抗体的发生率为31%(52例中的16例)。在总共48例发生或出现同种免疫的患者中,92%(48例中的44例)有阳性风险史。10例具有大于70%的板型反应性(PRA)的广泛多特异性HLA抗体的患者需要输注HLA匹配的血小板。PRA较低的HLA抗体患者可接受随机供者血小板支持。2例患者产生了血小板特异性抗体,导致输血难治性,需要通过缺乏血小板特异性抗原选择血小板。使用预储存白细胞去除的红细胞和血小板,残余白细胞少于5×10⁶,95%的患者,包括既往有风险史或有低PRA的HLA抗体患者,在整个血小板减少期均可接受随机供者输血支持。

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