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心脏骤停后及治疗性低温期间的镇静

Sedation after cardiac arrest and during therapeutic hypothermia.

作者信息

Dell'Anna A M, Taccone F S, Halenarova K, Citerio G

机构信息

Department of Intensive Care, Erasme Hospital, Université Libre de Bruxelles, Route de Lennik, Bruxelles, Belgium -

出版信息

Minerva Anestesiol. 2014 Aug;80(8):954-62. Epub 2013 Dec 3.

Abstract

Mild therapeutic hypothermia (MTH) has improved neurological outcome of comatose patients after cardiac arrest (CA). Since the first clinical studies performed in this setting, sedation has always been associated with cooling procedures. The use of sedative drugs during MTH is required because it allows faster achievement and better maintenance of target temperature. Further studies are necessary to prove any potential neuroprotective effects of sedation after CA. No differences in clinical outcomes have been found among different drugs, except for those related to their intrinsic pharmacological properties: the association propofol/remifentanil provides a faster recovery of consciousness than midazolam/fentanyl but is associated with the need of more vasopressors to maintain stable hemodynamic. Moreover, pharmacokinetic properties of these drugs are often altered during MTH so that standard drug regimens could result in overdosing because of reduced clearance. Neuromonitoring could be helpful to titrate drugs' effects and detect earlier complications (i.e. seizure), while a wake-up test should be avoided during the first 24 hours after CA.

摘要

轻度治疗性低温(MTH)改善了心脏骤停(CA)后昏迷患者的神经学预后。自在此情况下开展首批临床研究以来,镇静一直与降温程序相关联。在MTH期间使用镇静药物是必要的,因为它能使目标温度更快达到并更好地维持。需要进一步研究以证实CA后镇静的任何潜在神经保护作用。除了与药物固有药理学特性相关的差异外,不同药物之间未发现临床预后有差异:丙泊酚/瑞芬太尼联合使用比咪达唑仑/芬太尼能使意识恢复更快,但需要更多血管升压药来维持稳定的血流动力学。此外,这些药物的药代动力学特性在MTH期间常发生改变,因此标准药物方案可能因清除率降低而导致用药过量。神经监测有助于调整药物效果并更早发现并发症(如癫痫发作),而在CA后的头24小时内应避免唤醒试验。

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