活化的凝血酶原复合物可能减轻临床脓毒性休克相关严重脓毒症脑病。
Drotrecogin alfa (activated) may attenuate severe sepsis-associated encephalopathy in clinical septic shock.
机构信息
Intensive Care Department, University Hospital, Vrije Universiteit Brussel, Laarbeeklaan 101, Brussels, Belgium.
出版信息
Crit Care. 2010;14(2):R54. doi: 10.1186/cc8947. Epub 2010 Apr 7.
INTRODUCTION
Sepsis-associated encephalopathy (SAE) is a diffuse cerebral dysfunction induced by the immuno-inflammatory response to infection. Elevated levels of the brain-specific S100B protein are present in many septic patients and reflect the severity of SAE. Adjunctive treatment with drotrecogin alfa (activated) (DrotAA), the human recombinant form of activated protein C, has been shown to improve mortality in patients with severe sepsis-induced organ failure. We studied the effect of DrotAA on S100B levels in patients with acute septic shock who presented with increased baseline values of this biomarker.
METHODS
All patients received standard goal-directed resuscitation treatment. Patients with pre-existing or acute neurological disorders were excluded. Based on the Glasgow coma scale (GCS), patients were classified into two groups: GCS >or= 13 and GCS <13. DrotAA was given as a continuous infusion of 24 microg/kg/h for 96 h. S100B was measured before sedation and the start of DrotAA (0 h) and at 32 h, 64 h and 96 h and at corresponding time points in patients not treated with DrotAA. The lower limit of normal was < 0.5 microg/L.
RESULTS
Fifty-four patients completed the study. S100B was increased in 29 (54%) patients. Twenty-four patients (9 with GCS >or= 13 and 15 with GCS <13) received DrotAA. S100B levels in DrotAA-treated patients with a GCS <13, though higher at baseline than in untreated subjects (1.21 +/- 0.22 microg/L vs. 0.95 +/- 0.12 microg/L; P = 0.07), progressively and significantly decreased during infusion (0.96 +/- 0.22 microg/L at 32 h, P = 0.3; 0.73 +/- 0.12 microg/L at 64 h, P < 0.05; and 0.70 +/- 0.13 microg/L at 96 h, P < 0.05 vs. baseline). This patient group had also significantly lower S100B values at 64 h and at 96 h than their untreated counterparts. In the patients with a GCS >or= 13, S100B levels were not influenced by DrotAA treatment.
CONCLUSIONS
S100B-positivity is present in more than half of the patients with septic shock. When increased S100B levels are used as a surrogate for SAE, adjunctive DrotAA treatment seems to beneficially affect the evolution of severe SAE as discriminated by an admission GCS <13.
简介
脓毒症相关性脑病(SAE)是由感染引起的免疫炎症反应导致的弥漫性脑功能障碍。许多脓毒症患者的脑特异性 S100B 蛋白水平升高,反映了 SAE 的严重程度。辅助使用人重组活化蛋白 C(DrotAA)可改善严重脓毒症引起的器官衰竭患者的死亡率。我们研究了 DrotAA 对伴有基线升高的急性脓毒性休克患者 S100B 水平的影响。
方法
所有患者均接受标准目标导向的复苏治疗。排除有既往或急性神经疾病的患者。根据格拉斯哥昏迷评分(GCS),患者分为两组:GCS≥13 和 GCS<13。给予 DrotAA 持续输注 24μg/kg/h,持续 96 小时。在镇静前和 DrotAA 开始时(0 小时)以及在 32 小时、64 小时和 96 小时测量 S100B,并在未接受 DrotAA 治疗的患者中在相应时间点测量 S100B。正常下限<0.5μg/L。
结果
54 例患者完成了研究。29 例(54%)患者 S100B 升高。24 例患者(9 例 GCS≥13,15 例 GCS<13)接受了 DrotAA 治疗。GCS<13 的 DrotAA 治疗患者的 S100B 水平虽然高于未治疗患者(1.21±0.22μg/L vs. 0.95±0.12μg/L;P=0.07),但在输注过程中逐渐显著降低(32 小时时 0.96±0.22μg/L,P=0.3;64 小时时 0.73±0.12μg/L,P<0.05;96 小时时 0.70±0.13μg/L,P<0.05 vs. 基线)。该患者组在 64 小时和 96 小时的 S100B 值也明显低于未治疗组。GCS≥13 的患者中,DrotAA 治疗对 S100B 水平没有影响。
结论
脓毒性休克患者中超过一半的患者 S100B 阳性。当 S100B 水平升高用作 SAE 的替代指标时,辅助使用 DrotAA 治疗似乎对以入院时 GCS<13 区分的严重 SAE 的进展有益。
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