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I am the 9%: Making the case for whole-blood platelets

机译:我占9%:为全血血小板辩护

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SYNOPSIS Over the last 15 years, there has been a trend in the United States towards the increasing use of apheresis platelet (AP) concentrates over whole-blood-derived platelets (WBP). Although 1-h- and 24-h-corrected count increments tend to be higher with AP, this does not translate into improved haemostatic efficiency when used to prevent bleeding in haematology/oncology patients. WBP expose the recipient to more donors than apheresis products. However, recent studies have shown no significant differences in the rates of bacterial contamination, human leukocyte antigen alloimmunisation, RhD alloimmunisation, transfusion-related acute lung injury or febrile non-haemolytic transfusion reactions between these two products. Given the overall low rates of virally contaminated units in the era of nucleic acid testing and rigorous donor screening, the difference in donor exposures of 4-6 vs 1 has minimal clinical relevance. Although studies point to a marginally increased risk of donor adverse events associated with WBP, the absolute risk is too miniscule to act as a deterrent to making whole-blood donations. Both types of platelet concentrates should therefore be considered clinically equivalent; in this light, the most responsible use of the community donor resource pool, which both optimises the utility of a whole-blood donation and meets the clinical needs of thrombocytopenic recipients, is to have a mix of both types of platelet products so as to mitigate the risk of shortages.
机译:提要在过去的15年中,美国的趋势是越来越多地使用单采血浆血小板(AP)浓缩物而不是全血血小板(WBP)。尽管使用AP进行1小时和24小时校正的计数增量往往更高,但是当用于预防血液学/肿瘤学患者的出血时,这并不能提高止血效率。 WBP向接受者提供的捐献者多于血液分离产品。但是,最近的研究表明,这两种产品之间的细菌污染,人类白细胞抗原同种免疫,RhD同种免疫,输血相关的急性肺损伤或发热性非溶血性输血反应的速率均无显着差异。鉴于在核酸检测和严格的供体筛选时代,病毒污染单位的总体患病率较低,因此供体暴露的4-6比1的差异与临床相关性最小。尽管研究指出与WBP相关的供体不良事件的风险略有增加,但绝对风险却很小,不足以阻止全血捐赠。因此,两种血小板浓缩物在临床上均应视为同等的。有鉴于此,对社区捐赠者资源库的最负责任的使用既可以优化全血捐赠的使用,又可以满足血小板减少受体的临床需求,将两种类型的血小板产品混合使用,以减轻短缺的风险。

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