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血小板输注的临床方面。

Clinical aspects of platelet transfusions.

作者信息

Murphy M F, Waters A H

机构信息

Department of Haematology, St Bartholomew's Hospital and Medical College, London, UK.

出版信息

Blood Coagul Fibrinolysis. 1991 Apr;2(2):389-96. doi: 10.1097/00001721-199104000-00026.

Abstract

Refractoriness is the most important complication of platelet transfusion therapy, occurring in about 50% of patients receiving repeated transfusions. The major causes are HLA alloimmunization and non-immune platelet consumption associated with clinical factors such as septicaemia. DIC and splenomegaly. Initial management of alloimmunized patients who are refractory to platelet transfusions from random donors is the use of HLA-matched platelet transfusions, which improve responses to transfusions in about 65% of patients. It may be difficult to provide effective platelet transfusion support for alloimmunized patients not responding to HLA-matched transfusions. There has been much interest in methods for the prevention of HLA alloimmunization. Primary HLA alloimmunization is dependent on the presence of HLA class II antigen-bearing cells in transfusions; pure platelet transfusions are non-immunogenic as platelets only express HLA class I antigens. The use of leucocyte-depleted blood components in multitransfused patients has resulted in a reduction in HLA alloimmunization and platelet refractioness. Improvements in the techniques for leucocyte-depletion of red cell and platelet concentrates and the possibility of inactivation of HLA class II antigen-bearing cells by UV irradiation makes prevention of alloimmunization an attainable goal.

摘要

血小板输注治疗最重要的并发症是输注无效,约50%接受反复输血的患者会出现这种情况。主要原因是HLA同种免疫以及与败血症、弥散性血管内凝血和脾肿大等临床因素相关的非免疫性血小板消耗。对于随机供者血小板输注无效的同种免疫患者,初始治疗方法是使用HLA配型相合的血小板输注,约65%的患者对这种输注的反应会有所改善。对于对HLA配型相合输注无反应的同种免疫患者,可能难以提供有效的血小板输注支持。人们对预防HLA同种免疫的方法非常感兴趣。原发性HLA同种免疫取决于输注中是否存在携带HLAⅡ类抗原的细胞;纯血小板输注不具有免疫原性,因为血小板仅表达HLAⅠ类抗原。在多次输血的患者中使用去除白细胞的血液成分,已使HLA同种免疫和血小板输注无效的情况有所减少。红细胞和血小板浓缩物白细胞去除技术的改进,以及通过紫外线照射使携带HLAⅡ类抗原的细胞失活的可能性,使得预防同种免疫成为一个可以实现的目标。

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