Ma Shuai, Lin Yuli, Deng Bo, Zheng Yin, Hao Chuanming, He Rui, Ding Feng
Division of Nephrology & Unit of Critical Nephrology, Shanghai Ninth People's Hospital, School of Medicine, Shanghai Jiaotong University, 639 Zhizaoju Road, Shanghai, 200011, China.
Division of Nephrology, Huashan Hospital, Fudan University, Shanghai, 200040, China.
Intensive Care Med Exp. 2016 Dec;4(1):23. doi: 10.1186/s40635-016-0097-y. Epub 2016 Jul 22.
The endothelium is a potentially valuable target for sepsis therapy. We have previously studied an extracorporeal endothelial cell therapy system, called the endothelial bioreactor (EBR), which prolonged the survival time of endotoxemia sepsis in swine. To further study of the therapeutic effects and possible mechanisms, we established a miniature EBR system for septic rats induced by cecal ligation and puncture (CLP).
In the miniature EBR system, the extracorporeal circulation first passed through a mini-hemofilter, and the ultrafiltrate (UF) was separated, then the UF passed through an EBR (a 1-mL cartridge containing approximately 2 × 10(6) endothelial cells grown on microcarriers) and interact with endothelial cells. Eighteen hours after CLP, the rats were treated for 4 h with this extracorporeal system containing either endothelial cells (EBR group) or no cells (sham EBR group). Physiologic and biochemical parameters, cytokines, endothelial functions, and 7-day survival time were monitored. In vitro, the pulmonary endothelial cells of the septic rats were treated with the EBR system and the resulting changes in their functions were monitored.
The EBR system ameliorated CLP-induced sepsis compared with the sham EBR system. After CLP, the 7-day survival rate of sham-treated rats was only 25.0 %, while in the EBR-treated group, it increased to 57.1 % (p = 0.04). The EBR system protected the liver and renal function and ameliorated the kidney and lung injury. Meanwhile, this therapy reduced pulmonary vascular leakage and alleviated the infiltration of inflammatory cells in the lungs, especially neutrophils. Furthermore, after the EBR treatment both in vivo and in vitro, the expression of intercellular adhesion molecule-1 and the secretion of CXCL1 and CXCL2 of pulmonary endothelium decreased, which helped to alleviate the adhesion and chemotaxis of neutrophils. In addition, the EBR system decreased CD11b expression and intracellular free calcium level of peripheral blood neutrophils, modulated the activation of these neutrophils.
The EBR system significantly ameliorated CLP-induced sepsis and improved survival and organ functions. Compared with the sham EBR system, this extracorporeal endothelial therapy may be involved in modulating the function of pulmonary endothelial cells, reducing the adhesion and chemotaxis of neutrophil, and modulating the activation of peripheral blood neutrophils.
内皮细胞是脓毒症治疗中一个潜在的重要靶点。我们之前研究了一种体外内皮细胞治疗系统,称为内皮生物反应器(EBR),它延长了猪内毒素血症脓毒症的存活时间。为了进一步研究其治疗效果及可能机制,我们建立了一种用于盲肠结扎穿孔(CLP)诱导的脓毒症大鼠的微型EBR系统。
在微型EBR系统中,体外循环首先通过一个微型血液滤过器,分离出超滤液(UF),然后UF通过一个EBR(一个1毫升的柱体,包含在微载体上生长的约2×10⁶个内皮细胞)并与内皮细胞相互作用。CLP术后18小时,用这个包含内皮细胞的体外系统(EBR组)或不含细胞的体外系统(假EBR组)对大鼠进行4小时治疗。监测生理和生化参数、细胞因子、内皮功能及7天存活时间。在体外,用EBR系统处理脓毒症大鼠的肺内皮细胞,并监测其功能的变化。
与假EBR系统相比,EBR系统改善了CLP诱导的脓毒症。CLP术后,假治疗大鼠的7天存活率仅为25.0%,而EBR治疗组则增至57.1%(p = 0.04)。EBR系统保护了肝肾功能,改善了肾和肺损伤。同时,该治疗减少了肺血管渗漏,减轻了肺内炎症细胞浸润,尤其是中性粒细胞。此外,EBR体内和体外治疗后,肺内皮细胞间黏附分子-1的表达以及CXCL1和CXCL2的分泌减少,这有助于减轻中性粒细胞的黏附和趋化作用。另外,EBR系统降低了外周血中性粒细胞的CD11b表达和细胞内游离钙水平,调节了这些中性粒细胞的活化。
EBR系统显著改善了CLP诱导的脓毒症,提高了存活率和器官功能。与假EBR系统相比,这种体外内皮治疗可能参与调节肺内皮细胞功能,减少中性粒细胞的黏附和趋化作用,并调节外周血中性粒细胞的活化。
Zotero 插件
