Court Olivier, Kumar Aseem, Parrillo Joseph E, Kumar Anand
Section of Critical Care Medicine, Health Sciences Center, University of Manitoba, Winnipeg, Canada.
Crit Care. 2002 Dec;6(6):500-8. doi: 10.1186/cc1822. Epub 2002 Sep 12.
Myocardial dysfunction frequently accompanies severe sepsis and septic shock. Whereas myocardial depression was previously considered a preterminal event, it is now clear that cardiac dysfunction as evidenced by biventricular dilatation and reduced ejection fraction is present in most patients with severe sepsis and septic shock. Myocardial depression exists despite a fluid resuscitation-dependent hyperdynamic state that typically persists in septic shock patients until death or recovery. Cardiac function usually recovers within 7-10 days in survivors. Myocardial dysfunction does not appear to be due to myocardial hypoperfusion but due to circulating depressant factors, including the cytokines tumor necrosis factor alpha and IL-1beta. At a cellular level, reduced myocardial contractility seems to be induced by both nitric oxide-dependent and nitric oxide-independent mechanisms. The present paper reviews both the clinical manifestations and the molecular/cellular mechanisms of sepsis-induced myocardial depression.
心肌功能障碍常伴随严重脓毒症和脓毒性休克。虽然心肌抑制以前被认为是濒死事件,但现在很清楚,大多数严重脓毒症和脓毒性休克患者存在双心室扩张和射血分数降低所证明的心脏功能障碍。尽管脓毒性休克患者通常会持续存在依赖液体复苏的高动力状态直至死亡或康复,但仍存在心肌抑制。幸存者的心脏功能通常在7 - 10天内恢复。心肌功能障碍似乎不是由于心肌灌注不足,而是由于循环抑制因子,包括细胞因子肿瘤坏死因子α和白细胞介素-1β。在细胞水平上,心肌收缩力降低似乎是由一氧化氮依赖性和非一氧化氮依赖性机制共同诱导的。本文综述了脓毒症诱导的心肌抑制的临床表现以及分子/细胞机制。
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