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炎症、脓毒症和凝血系统。

Inflammation, Sepsis, and the Coagulation System.

机构信息

Department of Laboratory Medicine, Faculty of Medicine, University of Debrecen, Debrecen, Hungary.

出版信息

Hamostaseologie. 2024 Aug;44(4):268-276. doi: 10.1055/a-2202-8544. Epub 2024 Feb 14.

Abstract

Sepsis has been a major health problem for centuries and it is still the leading cause of hospital deaths. Several studies in the past decades have identified numerous biochemical abnormalities in severe cases, and many of these studies provide evidence of the perturbation of the hemostatic system. This can result in complications, such as disseminated intravascular coagulation that can lead to multiorgan failure. Nevertheless, large clinical studies have demonstrated that the simple approach of inhibiting the coagulation processes by any means fails to provide significant improvement in the survival of septic patients. A cause of this failure could be the fact that in sepsis the major clinical problems result not primarily from the presence of the infective agent or enhanced coagulation but from the complex dysregulated systemic host response to pathogens. If this overt reaction is not fully deciphered, appropriate interference is highly unlikely and any improvement by conventional therapeutic interventions would be limited. Cellular activation in sepsis can be targeted by novel approaches like inhibition of the heterotypic cellular interactions of blood cells by targeting surface receptors or posttranscriptional control of the hemostatic system by noncoding ribonucleic acid (RNA) molecules. Stable RNA molecules can affect the expression of several proteins. Thus, it can be anticipated that modulation of microRNA production would result in a multitude of effects that may be beneficial in septic cases. Here, we highlight some of the recent diagnostic possibilities and potential novel routes of the dysregulated host response.

摘要

败血症是几个世纪以来的一个主要健康问题,它仍然是医院死亡的主要原因。过去几十年的几项研究已经确定了严重病例中许多生化异常,其中许多研究为凝血系统失调提供了证据。这可能导致并发症,如弥散性血管内凝血,可导致多器官衰竭。然而,大型临床研究表明,通过任何手段抑制凝血过程的简单方法并不能显著提高败血症患者的生存率。这种失败的一个原因可能是,在败血症中,主要的临床问题主要不是由感染因子或增强的凝血引起的,而是由宿主对病原体的复杂失调全身反应引起的。如果没有完全破译这种明显的反应,就不可能进行适当的干扰,传统治疗干预的任何改善都将受到限制。败血症中的细胞激活可以通过新型方法来靶向,例如通过靶向表面受体抑制血细胞的异型细胞相互作用,或通过非编码 RNA(RNA)分子对凝血系统进行转录后控制。稳定的 RNA 分子可以影响几种蛋白质的表达。因此,可以预期,微 RNA 产生的调节将导致许多有益的效果,在败血症病例中可能有益。在这里,我们强调了一些最近的诊断可能性和失调宿主反应的潜在新途径。

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