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输注来自慢性粒细胞白血病供者的白细胞后,输血后粒细胞计数持续增加。

Sustained post-transfusion granulocyte count increments following transfusion of leukocytes obtained from donors with chronic myelogenous leukemia.

作者信息

Schiffer C A, Aisner J, Dutcher J P, Wiernik P H

出版信息

Am J Hematol. 1983 Aug;15(1):65-74. doi: 10.1002/ajh.2830150108.

Abstract

Leukocyte transfusions from patients with chronic myelogenous leukemia (CML) and elevated WBC counts were given to 14 patients with acute leukemia for the treatment of 16 infectious episodes. The WBCs were not irradiated to determine if engraftment with production of granulocytes would occur following infusion of immature myeloid elements. No recipient was alloimmunized by clinical and serologic criteria. High leukocyte yields were obtained using a variety of differential centrifugation techniques with a mean WBC yield/transfusion of 95 X 10(9) (range 19-275). A mean of 2.5 transfusions (range 1-11) were administered/recipient with a mean total dose of 235 X 10(9) WBC/transfusion episode (range 50-590). Seven patients had granulocyte counts greater than 500/microliters for four or more days (range 4-11 days) following the last transfusion. Ph1 chromosomes were documented in 2 of 4 patients tested 2-8 days following transfusion. Leukocyte alkaline phosphatase scores were increased (greater than 150) in 5/5 recipients tested post-transfusion demonstrating that production of this enzyme can be induced in CML granulocytes. Except for one severe transfusion reaction, there were no significant side effects and no recipient developed signs of graft versus host disease. All patients with sustained increments demonstrated rapid clinical improvement including 3 severely infected, poor risk patients undergoing initial induction therapy. These 3 patients all achieved complete remission with no evidence of the Ph1 chromosome. Because of the high dose of WBC which can be collected and the salutary effect of continued leukocyte production, CML WBC may be the preparation of choice for selected, non-alloimmunized, severely infected patients.

摘要

将慢性粒细胞白血病(CML)患者且白细胞计数升高的白细胞输注给14例急性白血病患者,以治疗16次感染发作。未对白细胞进行辐照,以确定输注未成熟髓系细胞后是否会发生粒细胞生成的植入。根据临床和血清学标准,没有接受者发生同种免疫。使用多种差速离心技术获得了高白细胞产量,每次输血的平均白细胞产量为95×10⁹(范围为19 - 275)。每位接受者平均输注2.5次(范围为1 - 11次),每次输血发作的平均总剂量为235×10⁹白细胞(范围为50 - 590)。7例患者在最后一次输血后4天或更长时间(范围为4 - 11天)粒细胞计数大于500/微升。在输血后2 - 8天检测的4例患者中有2例记录到Ph1染色体。5例输血后检测的接受者白细胞碱性磷酸酶评分升高(大于150),表明这种酶可在CML粒细胞中诱导产生。除了1次严重的输血反应外,没有明显的副作用,也没有接受者出现移植物抗宿主病的迹象。所有白细胞持续增加的患者临床症状迅速改善,包括3例正在接受初始诱导治疗、严重感染且预后不良的患者。这3例患者均实现完全缓解,且没有Ph1染色体的证据。由于可以采集高剂量的白细胞以及持续白细胞生成的有益效果,CML白细胞可能是选定的、未发生同种免疫的、严重感染患者的首选制剂。

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