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首页> 外文期刊>Transfusion: The Journal of the American Association of Blood Banks >Measurement of the absolute immature platelet number reflects marrow production and is not impacted by platelet transfusion
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Measurement of the absolute immature platelet number reflects marrow production and is not impacted by platelet transfusion

机译:绝对未成熟血小板数的测量反映了骨髓的产生,不受血小板输注的影响

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Background The ability to distinguish increased platelet (PLT) destruction from PLT hypoproduction is important in the care of patients with marrow failure syndromes and patients receiving high-dose chemotherapy. The measurement of immature circulating PLTs based on RNA content using an automated counter is now feasible. This study evaluated the impact of recent PLT transfusion on measurement of immature PLT variables. Study Design and Methods The immature PLT fraction (IPF) and absolute immature PLT number (AIPN) were measured using a hematology analyzer before and after PLT transfusion in nine transfusion-dependent patients with marrow failure secondary to aplastic anemia, myelodysplasia, or transplantation conditioning. IPF and AIPN were also measured serially over 5 days of storage in three plateletpheresis components collected from normal donors. Results PLT transfusion did not significantly change the mean AIPN in transfused patients. In contrast, IPF decreased significantly from 6.6 ± 4.6% on Day -1 to 2.3 ± 1.4% on Day 0 before returning to 4.3 ± 2.3% on Day +1. In the PLT component, AIPN and IPF% increased significantly over 5 days of storage, most likely due to an artifact of the staining and detection process for stored PLTs, no longer detected in vivo once the PLTs were transfused. Conclusion PLT transfusion decreases the IPF due to the resultant increase in circulating PLT count. However, PLT transfusion does not change the circulating AIPN, validating this assay as a reflection of ongoing PLT production by the marrow in various clinical settings, regardless of proximity to PLT transfusion.
机译:背景技术区分血小板增多(PLT)破坏与PLT低产的能力在治疗骨髓衰竭综合征和接受大剂量化疗的患者中很重要。使用自动计数器基于RNA含量测量未成熟循环PLT现在是可行的。这项研究评估了最近的PLT输血对未成熟PLT变量的测量的影响。研究设计和方法在9例因再生障碍性贫血,骨髓增生异常或移植条件导致的骨髓衰竭的输血依赖患者中,在输血前后使用血液分析仪测量了未成熟PLT分数(IPF)和绝对未成熟PLT数(AIPN)。 IPF和AIPN还在从正常供体收集的三种血小板减少成分中储存5天以上进行了连续测量。结果PLT输注并没有显着改变输血患者的平均AIPN。相反,IPF从第-1天的6.6±4.6%显着下降到第0天的2.3±1.4%,然后在第+1天返回4.3±2.3%。在PLT组分中,AIPN和IPF%在保存5天后显着增加,这很可能是由于保存的PLT染色和检测过程的伪影所致,一旦输注了PLT,就不再在体内检测到。结论PLT输注降低IPF的原因是循环PLT计数增加。但是,PLT输注并不会改变循环的AIPN,从而验证了该测定方法反映了骨髓在各种临床情况下持续进行PLT产生的结果,无论是否接近PLT输注。

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