Clinic for Anesthesiology, University of Munich, Max-Lebsche-Platz 32, D-81377 Munich, Germany.
Anesth Analg. 2010 Mar 1;110(3):702-7. doi: 10.1213/ANE.0b013e3181c92a5c. Epub 2009 Dec 30.
Blood loss after cardiac surgery can be caused by acquired platelet dysfunction after cardiopulmonary bypass. Monitoring of platelet function is clinically important for the identification of patients experiencing such platelet dysfunction. 1-Deamino-8-D-arginine vasopressin (desmopressin acetate, DDAVP) has been shown to augment platelet function and to reduce blood loss in patients with platelet dysfunction. In this study, we examined the feasibility of whole blood multiple electrode aggregometry (MEA) for the detection of cardiopulmonary bypass-induced platelet dysfunction and investigated its ability to monitor DDAVP treatment.
Fifty-eight consecutive patients with blood loss exceeding 150 mL/h in the first 2 consecutive hours after cardiac surgery were screened for suspected isolated platelet dysfunction. Twenty-two patients had suspected isolated platelet dysfunction and were enrolled in the study. Platelet dysfunction was assumed if conventional coagulation analyses (platelet count, activated partial thromboplastin time, international normalized ratio, and fibrinogen) did not show abnormal values as defined for transfusion of allogenic blood products, and no surgical cause of bleeding was suspected. Eleven patients received 0.3 microg/kg DDAVP, and 11 patients received no therapy in a nonrandomized manner. MEA was performed after stimulation with thrombin receptor-activating peptide (TRAPtest, 32 microM), adenosine diphosphate (ADPtest, 6.4 microM), and arachidonic acid (ASPItest, 0.5 mM) before and 2 hours after intervention. Conventional laboratory variables were recorded. The Mann-Whitney test was used to detect differences between the groups, and the Wilcoxon test was used to detect differences before and after intervention.
All enrolled patients showed platelet dysfunction that manifested as impaired platelet aggregation in MEA before intervention. After the intervention, platelet function improved in the DDAVP group (49 U [30/72 U], median [25th/75th percentile] postintervention vs 15 U [8/21 U] preintervention for the ASPItest [P < 0.001]; 35 U [24/54 U] vs 14 U [7/28 U] for the ADPtest [P = 0.002]; and 85 U [66/115 U] vs 64 U [26/88 U] for the TRAPtest [P = 0.007]). In contrast, MEA remained unchanged in the control group (22 U [10/50 U] postintervention vs 33 U [14/57 U] preintervention for the ASPItest [P = 0.175]; 17 U [12/20 U] vs 14 U [10/28 U] for the ADPtest [P = 0.147]; and 65 U [41/89 U] vs 57 U [30/91 U] for the TRAPtest [P = 0.123]).
Impaired platelet function after cardiac surgery can be assessed at the bedside using MEA. The effect of DDAVP on impaired platelet function can also be detected as significant improvement in platelet aggregation to all activators. This device might be helpful for the identification of patients who may benefit from DDAVP therapy.
体外循环后获得性血小板功能障碍可导致心脏手术后出血。血小板功能监测对于识别发生血小板功能障碍的患者具有重要的临床意义。1-脱氨基-8-D-精氨酸血管加压素(醋酸去氨加压素,DDAVP)已被证明可增强血小板功能并减少血小板功能障碍患者的出血。在这项研究中,我们检查了全血多电极聚集仪(MEA)检测体外循环诱导的血小板功能障碍的可行性,并研究了其监测 DDAVP 治疗的能力。
连续筛选 58 例心脏手术后前 2 小时内每小时失血超过 150 mL/h 的患者,以怀疑孤立性血小板功能障碍。22 例患者有疑似孤立性血小板功能障碍,并被纳入研究。如果常规凝血分析(血小板计数、活化部分凝血活酶时间、国际标准化比值和纤维蛋白原)未显示异常值(定义为输注同种异体血液制品),且无手术出血原因,则假定存在血小板功能障碍。11 例患者接受了 0.3 μg/kg DDAVP,11 例患者未接受治疗(非随机)。在干预前和干预后 2 小时,用血栓素受体激活肽(TRAPtest,32 μM)、二磷酸腺苷(ADPtest,6.4 μM)和花生四烯酸(ASPItest,0.5 mM)刺激后进行 MEA。记录常规实验室变量。使用 Mann-Whitney 检验检测组间差异,使用 Wilcoxon 检验检测干预前后差异。
所有入组患者在干预前的 MEA 中均表现出血小板功能障碍,表现为血小板聚集受损。干预后,DDAVP 组血小板功能改善(ASPItest 检测,干预后 49 U [30/72 U],中位数 [25/75 分位] vs 干预前 15 U [8/21 U];P < 0.001;ADPtest 检测,35 U [24/54 U] vs 14 U [7/28 U];P = 0.002;TRAPtest 检测,85 U [66/115 U] vs 64 U [26/88 U];P = 0.007)。相比之下,MEA 在对照组中无变化(ASPItest 检测,干预后 22 U [10/50 U] vs 干预前 33 U [14/57 U];P = 0.175;ADPtest 检测,17 U [12/20 U] vs 14 U [10/28 U];P = 0.147;TRAPtest 检测,65 U [41/89 U] vs 57 U [30/91 U];P = 0.123)。
心脏手术后的血小板功能障碍可以通过 MEA 在床边进行评估。DDAVP 对血小板功能障碍的作用也可以通过所有激活剂的血小板聚集的显著改善来检测。该设备可能有助于识别可能受益于 DDAVP 治疗的患者。
