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使用去白细胞血小板浓缩物预防血小板输注无效和原发性HLA同种免疫:一项前瞻性随机试验。

Use of leukocyte-depleted platelet concentrates for the prevention of refractoriness and primary HLA alloimmunization: a prospective, randomized trial.

作者信息

van Marwijk Kooy M, van Prooijen H C, Moes M, Bosma-Stants I, Akkerman J W

机构信息

Department of Immuno-Hematology, University Hospital Utrecht, The Netherlands.

出版信息

Blood. 1991 Jan 1;77(1):201-5.

PMID:1984797
Abstract

Compared with conventional transfusion regimes a strong reduction in HLA alloimmunization and refractoriness to platelet transfusions is obtained when both red blood cell concentrates (RBCs) and platelet concentrates (PCs) are depleted of leukocytes by filtration. Because most of the leukocyte contamination is introduced by transfusion of RBCs, filtration of RBCs appears rational, but uncertainty exists regarding the degree of leukocyte-depletion of PCs needed for the prevention of HLA alloimmunization and refractoriness. We conducted a prospective trial and randomized patients with acute leukemia to receive leukocyte-depleted PCs prepared either by centrifugation (mean leukocyte count 35 x 10(6)/PC of 6 U) or by filtration (mean leukocyte count less than 5 x 10(6)/PC of 6 U). Both groups received RBCs that were filtered after prior removal of the buffy coat. Clinical refractoriness occurred in 46% (12 of 26) of the evaluable patients that were transfused with centrifuged PCs and only in 11% (3 of 27) in the filtered group (P less than .005). De novo anti-HLA antibodies were detected in 42% (11 of 26) patients in the centrifuged group and only in 7% (2 of 27) of the patients receiving filtered PCs (P less than .004). In 8 of 11 alloimmunized patients in the centrifuged group antibodies were detected in the first 4 weeks of transfusion therapy while none of the patients in the filtered group became immunized against HLA antigens during that period. We conclude that for the prevention of HLA alloimmunization and refractoriness to platelet transfusions from random donors, both RBCs and PCs have to be leukocyte-depleted by filtration.

摘要

与传统输血方案相比,当红细胞浓缩物(RBCs)和血小板浓缩物(PCs)均通过过滤去除白细胞时,HLA同种免疫和对血小板输注的不应性会显著降低。由于大多数白细胞污染是由RBCs输注引入的,因此对RBCs进行过滤似乎是合理的,但对于预防HLA同种免疫和不应性所需的PCs白细胞去除程度仍存在不确定性。我们进行了一项前瞻性试验,将急性白血病患者随机分为两组,分别接受通过离心制备的白细胞去除PCs(平均白细胞计数为35×10⁶/6单位的PC)或通过过滤制备的白细胞去除PCs(平均白细胞计数小于5×10⁶/6单位的PC)。两组均接受在去除白膜层后过滤的RBCs。接受离心制备PCs输注的可评估患者中,46%(26例中的12例)出现临床不应性,而过滤组仅为11%(27例中的3例)(P<0.005)。离心组42%(26例中的11例)患者检测到新生抗HLA抗体,而接受过滤PCs的患者中仅7%(27例中的2例)检测到(P<0.004)。离心组11例同种免疫患者中有8例在输血治疗的前4周检测到抗体,而过滤组在此期间无患者对HLA抗原产生免疫。我们得出结论,为预防随机供体血小板输注的HLA同种免疫和不应性,RBCs和PCs均必须通过过滤去除白细胞。

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