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首页> 外文期刊>Vox Sanguinis: International Journal of Blood Transfusion and Immunohaematology >Agonist‐induced platelet reactivity correlates with bleeding in haemato‐oncological patients
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Agonist‐induced platelet reactivity correlates with bleeding in haemato‐oncological patients

机译:受体激动剂诱导血小板反应性相关出血进入haemato非肿瘤病人

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摘要

Background and objective Prophylactic platelet transfusions are administered to prevent bleeding in haemato‐oncological patients. However, bleeding still occurs, despite these transfusions. This practice is costly and not without risk. Better predictors of bleeding are needed, and flow cytometric evaluation of platelet function might aid the clinician in identifying patients at risk of bleeding. This evaluation can be performed within the hour and is not hampered by low platelet count. Our objective was to assess a possible correlation between bleeding and platelet function in thrombocytopenic haemato‐oncological patients. Materials and Methods Inclusion was possible for admitted haemato‐oncology patients aged 18?years and above. Furthermore, an expected need for platelet transfusions was necessary. Bleeding was graded according to the WHO bleeding scale. Platelet reactivity to stimulation by either adenosine diphosphate ( ADP ), cross‐linked collagen‐related peptide ( CRP ‐ xL ), PAR 1‐ or PAR 4‐activating peptide ( AP ) was measured using flow cytometry. Results A total of 114 evaluations were available from 21 consecutive patients. Platelet reactivity in response to stimulation by all four studied agonists was inversely correlated with significant bleeding. Odds ratios ( OR ) for bleeding were 0·28 for every unit increase in median fluorescence intensity ( MFI ) [95% confidence interval ( CI ) 0·11–0·73] for ADP ; 0·59 [0·40–0·87] for CRP ‐ xL ; 0·59 [0·37–0·94] for PAR 1‐ AP ; and 0·43 [0·23–0·79] for PAR 4‐ AP . The platelet count was not correlated with bleeding ( OR 0·99 [0·96–1·02]). Conclusion Agonist‐induced platelet reactivity was significantly correlated to bleeding. Platelet function testing could provide a basis for a personalized transfusion regimen, in which platelet transfusions are limited to those at risk of bleeding.
机译:背景和目的预防性血小板输血管理,以防止出血进入haemato非肿瘤病人。出血仍然发生,尽管这些输血。没有风险的。需要和流量仪的评价血小板功能可以帮助临床医生识别患者出血的风险。可以在一个小时内执行和评估不受低血小板计数。目的是评估可能的相关性出血和血小板功能之间血小板减少性haemato肿瘤病人。材料和方法包含是可能的承认haemato检测肿瘤患者18岁?及以上。血小板输血是必要的。分级根据世界卫生组织的出血。血小板反应性的刺激二磷酸腺苷(ADP)、交叉链接胶原蛋白量相关肽(CRP检测xL), 1量或持平PAR 4激活肽(美联社)测量使用流式细胞仪。评估可以从连续21病人。刺激,所有四个研究受体激动剂负相关显著的出血。优势比(或)出血0·28了增加每单位平均荧光强度(MFI)[95%可信区间(CI)没有与出血(或0·99[96 - 1·0·02])。反应性显著相关出血。一个个性化的输血疗法的基础,在血小板输血是有限的这些出血的风险。

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