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Acute respiratory distress syndrome: pharmacological treatment options in development.

机译:急性呼吸窘迫综合征:正在开发中的药物治疗选择。

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摘要

The acute respiratory distress syndrome (ARDS) is a clinical syndrome with primarily supportive management options. Despite extensive basic and clinical investigations, multiple pharmacological and nonpharmacological modalities have been unsuccessful in decreasing mortality. Nonetheless, these efforts have substantially heightened our understanding of ARDS pathophysiology. Investigators continue to create new and more complex therapeutic strategies that may have significant clinical impact. Several pharmacological agents for ARDS are in development and have shown either great promise or are at most, under phase II evaluation. The order in which therapeutic options are presented in this review highlights therapeutic options other than the anti-inflammatory approach. In addition to the anti-inflammatory category, vasodilators, surfactant therapy, immunonutrition and partial liquid ventilation are all being evaluated. Within the anti-inflammatory category. new mechanistic approaches include the 'anti-inflammatory nature' of interleukin-10, the inhibitory aspects of lysophosphatidic acid on endothelial cell permeability, and the use of recombinant human anti-coagulant proteins (activated protein C and tissue factor pathway inhibitor) to reduce the inflammatory cycle that contributes to microvascular thrombi. Previous work with surfactant in ARDS had its limitations, however, these trials were of sufficient success to spawn 2 new synthetic compounds. These new synthetic surfactants incorporate mixtures of phosphatidylcholine and phosphatidylglycerol (the key phospholipids within endogenous surfactant) and either recombinant surfactant protein C or an analogue of surfactant protein B. Recently, the ARDS Network's low tidal volume study has broken the cycle of decades of negative ARDS trials and demonstrated an improvement in mortality. Through better mechanistic approach and study design, investigator compliance with exclusion criteria, and better understanding of the complexities of patient management, the next pharmacological ARDS trials will hopefully be successful and lead to further reductions in patient mortality.
机译:急性呼吸窘迫综合征(ARDS)是一种临床综合征,主要有支持性治疗选择。尽管进行了广泛的基础和临床研究,但多种药理学和非药理学方法仍未能成功降低死亡率。尽管如此,这些努力大大提高了我们对ARDS病理生理学的理解。研究人员继续创建可能具有重大临床影响的新的和更复杂的治疗策略。在II期评估中,有几种ARDS药理药物正在开发中,它们显示出了很大的希望,或者显示出最大的希望。在这篇综述中提出的治疗选择的顺序突出了除抗炎方法以外的治疗选择。除了抗炎药,还对血管扩张药,表面活性剂疗法,免疫营养和部分液体通气进行了评估。在消炎类内。新的机械方法包括白细胞介素10的“抗炎特性”,溶血磷脂酸对内皮细胞通透性的抑制作用,以及使用重组人抗凝蛋白(活化的C蛋白和组织因子途径抑制剂)降低促成微血管血栓的炎症周期。以前在ARDS中使用表面活性剂进行的工作有其局限性,但是,这些试验取得了足够的成功,可以生成2种新的合成化合物。这些新的合成表面活性剂结合了磷脂酰胆碱和磷脂酰甘油(内源性表面活性剂中的关键磷脂)和重组表面活性剂蛋白C或表面活性剂蛋白B的类似物的混合物。最近,ARDS网络的低潮气量研究打破了数十年来阴性ARDS的循环试验并证明死亡率有所改善。通过更好的机械方法和研究设计,研究者符合排除标准,以及更好地了解患者管理的复杂性,下一次药理学ARDS试验有望获得成功,并进一步降低患者死亡率。

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