Mitochondrial Pathophysiology Unit, Laboratory for Experimental Brain Research, Department of Clinical Sciences, Lund University, Sölvegatan 17, SE-221 84, Lund, Sweden.
Crit Care. 2010;14(6):R214. doi: 10.1186/cc9337. Epub 2010 Nov 24.
Mitochondrial dysfunction has been suggested as a contributing factor to the pathogenesis of sepsis-induced multiple organ failure. Also, restoration of mitochondrial function, known as mitochondrial biogenesis, has been implicated as a key factor for the recovery of organ function in patients with sepsis. Here we investigated temporal changes in platelet mitochondrial respiratory function in patients with sepsis during the first week after disease onset.
Platelets were isolated from blood samples taken from 18 patients with severe sepsis or septic shock within 48 hours of their admission to the intensive care unit. Subsequent samples were taken on Day 3 to 4 and Day 6 to 7. Eighteen healthy blood donors served as controls. Platelet mitochondrial function was analyzed by high-resolution respirometry. Endogenous respiration of viable, intact platelets suspended in their own plasma or phosphate-buffered saline (PBS) glucose was determined. Further, in order to investigate the role of different dehydrogenases and respiratory complexes as well as to evaluate maximal respiratory activity of the mitochondria, platelets were permeabilized and stimulated with complex-specific substrates and inhibitors.
Platelets suspended in their own septic plasma exhibited increased basal non-phosphorylating respiration (state 4) compared to controls and to platelets suspended in PBS glucose. In parallel, there was a substantial increase in respiratory capacity of the electron transfer system from Day 1 to 2 to Day 6 to 7 as well as compared to controls in both intact and permeabilized platelets oxidizing Complex I and/or II-linked substrates. No inhibition of respiratory complexes was detected in septic patients compared to controls. Non-survivors, at 90 days, had a more elevated respiratory capacity at Day 6 to 7 as compared to survivors. Cytochrome c increased over the time interval studied but no change in mitochondrial DNA was detected.
The results indicate the presence of a soluble plasma factor in the initial stage of sepsis inducing uncoupling of platelet mitochondria without inhibition of the electron transfer system. The mitochondrial uncoupling was paralleled by a gradual and substantial increase in respiratory capacity. This may reflect a compensatory response to severe sepsis or septic shock, that was most pronounced in non-survivors, likely correlating to the severity of the septic insult.
线粒体功能障碍被认为是导致脓毒症引起多器官衰竭的发病机制的一个因素。此外,已知线粒体功能的恢复,即线粒体生物发生,被认为是脓毒症患者器官功能恢复的关键因素。在这里,我们研究了发病后第一周内脓毒症患者血小板线粒体呼吸功能的时间变化。
在入住重症监护病房的 48 小时内,从 18 名严重脓毒症或感染性休克患者的血液样本中分离血小板。随后在第 3 天至第 4 天和第 6 天至第 7 天采集样本。18 名健康献血者作为对照。通过高分辨率呼吸测量法分析血小板线粒体功能。测定悬浮在自身血浆或磷酸盐缓冲盐水(PBS)葡萄糖中的有活力、完整血小板的内源性呼吸。此外,为了研究不同脱氢酶和呼吸复合物的作用,并评估线粒体的最大呼吸活性,对血小板进行了通透化处理,并使用复合物特异性底物和抑制剂进行了刺激。
悬浮在自身脓毒性血浆中的血小板与对照组和悬浮在 PBS 葡萄糖中的血小板相比,表现出增加的基础非磷酸化呼吸(状态 4)。与此平行的是,从第 1 天到第 2 天到第 6 天到第 7 天,电子传递系统的呼吸能力有了实质性的增加,与对照组相比,无论是在完整的还是通透化的血小板中,氧化 I 型和/或 II 型偶联底物时都是如此。与对照组相比,脓毒症患者中没有检测到呼吸复合物的抑制。90 天时的非幸存者在第 6 天至第 7 天的呼吸能力比幸存者更高。细胞色素 c 在研究期间增加,但未检测到线粒体 DNA 的变化。
这些结果表明,在脓毒症的初始阶段存在一种可溶性血浆因子,它诱导血小板线粒体解偶联而不抑制电子传递系统。线粒体解偶联伴随着呼吸能力的逐渐显著增加。这可能反映了对严重脓毒症或感染性休克的代偿反应,在非幸存者中最为明显,可能与脓毒症的严重程度相关。
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