感染性休克:一种微循环疾病。

IF 2.1
Daniel De Backer, Francesco Ricottilli, Gustavo A Ospina-Tascón
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引用次数: 31

摘要

回顾目的:本研究的目的是讨论感染性休克中微血管功能障碍的意义。最近的发现:败血症的复苏主要集中在全身血流动力学和最近的外周灌注指数上。然而,中枢性微血管灌注在败血症中发生改变,尽管各种宏观血流动力学复苏目标正常化,但这些改变往往持续存在。内皮功能障碍是脓毒症病理生理的关键因素。它负责败血症引起的低血压。此外,内皮功能障碍还涉及炎症和凝血过程的激活,从而导致脓毒性反应的放大和器官功能障碍的发展。它还促进通透性的增加,主要是在静脉侧,并损害微血管灌注,从而损害组织氧合。微血管改变的特点是血流分布的异质性,充分灌注的区域靠近未灌注的区域,从而表征了感染性休克的分布性质。这种微血管改变具有深远的意义,因为它们与器官功能障碍和不良后果有关。此外,对治疗的反应是高度可变的,不能通过全身血流动力学评估来预测,因此不能通过经典的血流动力学工具来检测。微循环是脓毒症病理生理的关键因素。即使微循环靶向治疗尚未准备好,了解微血管功能障碍的过程对于防止在不有助于改善组织灌注的情况下追逐全身血流动力学变量是重要的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Septic shock: a microcirculation disease.

Purpose of review: The aim of this study was to discuss the implication of microvascular dysfunction in septic shock.

Recent findings: Resuscitation of sepsis has focused on systemic haemodynamics and, more recently, on peripheral perfusion indices. However, central microvascular perfusion is altered in sepsis and these alterations often persist despite normalization of various macro haemodynamic resuscitative goals. Endothelial dysfunction is a key element in sepsis pathophysiology. It is responsible for the sepsis-induced hypotension. In addition, endothelial dysfunction is also implicated involved in the activation of inflammation and coagulation processes leading to amplification of the septic response and development of organ dysfunction. It also promotes an increase in permeability, mostly at venular side, and impairs microvascular perfusion and hence tissue oxygenation.Microvascular alterations are characterized by heterogeneity in blood flow distribution, with adequately perfused areas in close vicinity to not perfused areas, thus characterizing the distributive nature of septic shock. Such microvascular alterations have profound implications, as these are associated with organ dysfunction and unfavourable outcomes. Also, the response to therapy is highly variable and cannot be predicted by systemic hemodynamic assessment and hence cannot be detected by classical haemodynamic tools.

Summary: Microcirculation is a key element in the pathophysiology of sepsis. Even if microcirculation-targeted therapy is not yet ready for the prime time, understanding the processes implicated in microvascular dysfunction is important to prevent chasing systemic hemodynamic variables when this does not contribute to improve tissue perfusion.

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