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Procalcitonin and C-reactive protein levels at admission as predictors of duration of acute brain dysfunction in critically ill patients

机译:入院时降钙素原和C反应蛋白水平可作为重症患者急性脑功能障碍持续时间的预测指标

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IntroductionNon-intensive care unit (ICU) cohorts have shown an association between inflammatory disturbances and delirium, though these relationships have not been studied in critically ill patients. This study sought to investigate the relationship between two inflammatory biomarkers, procalcitonin and C-reactive protein (CRP), and duration of acute brain dysfunction in ventilated patients.MethodsPatients enrolled in the Maximizing Efficacy of Targeted Sedation and Reducing Neurological Dysfunction (MENDS) trial were assessed daily for delirium using the Confusion Assessment Method-ICU. Plasma levels of procalcitonin and CRP were obtained within 24 hours of enrollment. Proportional odds logistic regression was used to examine the association between procalcitonin and CRP separately with delirium/coma-free days, adjusting for age, acute physiology score (APS) of the Acute Physiology And Chronic Health Evaluation (APACHE) II, sedation group (dexmedetomidine vs. lorazepam), and sepsis. Secondary analyses examined the association of these markers with other organ dysfunctions and 28-day survival.ResultsEighty-seven patients were included in this analysis. The median age of the patients was 60 years with APACHE II scores of 28; 68% had sepsis within 48 hours of admission. Higher levels of procalcitonin were associated with fewer delirium/coma-free days [odds ratio (OR), 0.5; 95% confidence interval (CI), 0.3 to 1.0; P = 0.04], whereas higher CRP levels showed trends towards fewer delirium/coma-free days (OR, 0.6; 95% CI, 0.3 to 1.1; P = 0.08). Similar relationships were found regardless of the presence of sepsis. No associations were found between procalcitonin or CRP with 28-day survival (P = 0.40 and 0.16, respectively).ConclusionsIn our pilot study, high baseline inflammatory biomarkers predicted prolonged periods of acute brain dysfunction, implicating inflammation as an important mechanism in the pathophysiology of delirium and coma during critical illness, irrespective of whether patients had sepsis or not.
机译:简介尽管重症患者尚未研究过这些关系,但非重症监护病房(ICU)队列却显示出炎症紊乱与del妄之间存在关联。本研究旨在探讨通气患者降钙素原和C反应蛋白(CRP)这两种炎性生物标志物与急性脑功能障碍持续时间之间的关系。方法参加有针对性镇静作用和减轻神经功能障碍(MENDS)疗效最大化的患者使用混淆评估方法(ICU)每天评估del妄。入组24小时内获得血浆降钙素原和CRP水平。采用比例比对数Logistic回归分析了降钙素和CRP与ir妄/无昏迷天数之间的关联,调整了年龄,急性生理和慢性健康评估(APACHE)II,镇静组(右美托咪定)的急性生理评分(APS)与劳拉西m)和败血症。二级分析检查了这些标志物与其他器官功能障碍和28天生存率的关联。结果本分析纳入了87例患者。患者的中位年龄为60岁,APACHE II评分为28。 68%的人在入院48小时内患有败血症。降钙素原水平越高,del妄/无昏迷天数越少[赔率(OR)为0.5; 95%置信区间(CI),0.3至1.0; P = 0.04],而较高的CRP水平则显示出减少del妄/无昏迷天数的趋势(OR为0.6; 95%CI为0.3至1.1; P = 0.08)。无论是否存在败血症,都发现了相似的关系。结论:降钙素原或CRP与28天生存率之间无关联(分别为P = 0.40和0.16)。结论在我们的初步研究中,高基线炎症生物标志物预示了急性脑功能障碍的时间延长,这暗示炎症是其病理生理的重要机制。危重疾病中的妄和昏迷,无论患者是否患有败血症。

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