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细胞因子驱动疾病的血液滤过:介质传递假说

Hemofiltration for cytokine-driven illnesses: the mediator delivery hypothesis.

作者信息

Di Carlo J V, Alexander S R

机构信息

Division of Pediatric Critical Care Medicine, Stanford University, 750 Welch Road Suite 315, Palo Alto, CA 94304, USA.

出版信息

Int J Artif Organs. 2005 Aug;28(8):777-86. doi: 10.1177/039139880502800803.

Abstract

Hemofiltration is evolving as an adjunctive therapy for sepsis and other forms of systemic inflammation. Designed as a substitute for lost renal function, it is sometimes employed prior to the onset of renal failure to facilitate the nonspecific clearance of pro-inflammatory mediators. Prevailing theories suggest that hemofiltration attenuates the immune response when a threshold amount of excess cytokine is removed at the semi-permeable membrane. In this article we introduce an alternative hypothesis, in which hemofiltration exerts its effect by reinvigorating lymphatic flow and function. Crystalloid "replacement" solution, as much as 48 to 72 liters daily, is infused to restore intravascular volume lost through production of ultrafiltrate. Partial redistribution into interstitium and lymph mobilizes inflammatory mediators and other proteins, cellular byproducts, excessive ground matrix, fragments of apoptotic cells and free DNA. These substances are then metabolized, scavenged or cleared at multiple sites, including the reticuloendothelial system, liver, kidney, erythrocyte, and hemofilter.

摘要

血液滤过正逐渐发展成为脓毒症及其他形式全身炎症的辅助治疗方法。它被设计用来替代丧失的肾功能,有时在肾衰竭发生前使用,以促进促炎介质的非特异性清除。流行理论认为,当在半透膜上去除阈值量的过量细胞因子时,血液滤过会减弱免疫反应。在本文中,我们提出了另一种假说,即血液滤过通过恢复淋巴流动和功能发挥其作用。每天输注多达48至72升的晶体“置换”溶液,以恢复因产生超滤液而损失的血管内容量。部分液体重新分布到间质和淋巴中,可动员炎症介质和其他蛋白质、细胞副产物、过多的细胞外基质、凋亡细胞碎片和游离DNA。这些物质随后在多个部位进行代谢、清除或滤过,包括网状内皮系统、肝脏、肾脏、红细胞和血液滤过器。

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