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Scavengers of hemoproteins as potential biomarkers for severe sepsis and septic shock

机译:血蛋白的清除剂作为严重脓毒症和脓毒症休克的潜在生物标志物

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Background Despite improvements in diagnosis, interventions and supportive care, mortality among sepsis patients is still high. Research of the past decade has attempted to identify biomarkers that can accurately discriminate sepsis from other diseases with comparable symptoms to improve diagnosis, but results have been lackluster. Recent studies have shown that hemoproteins and damage-associated molecular patterns (DAMPs) such as mitochondrial DNA (mtDNA) released as the result of hemolysis play an important role in the pathogenesis of sepsis. The aim of this study was to measure plasma levels of the indirect markers for hemoproteins hemopexin, haptoglobin and heme oxygenase-1 (HO-1) as well as the mitochondrial damage marker mtDNA in the plasma of a cohort of sepsis patients to determine the feasibility of their use as biomarkers in the diagnosis of sepsis. Methods Hemopexin, haptoglobin and HO-1 were measured in plasma by ELISA and mtDNA was measured by digital droplet PCR. Plasma levels of hemopexin, haptoglobin, HO-1 and mtDNA were measured in 32 patients with severe sepsis and 8 patients with septic shock at baseline and 4 days after admission to the ICU and in 20 healthy donors. Results Plasma levels of hemopexin were significantly lower and plasma levels of HO-1, haptoglobin and mtDNA were significantly higher in patients with severe sepsis and septic shock at baseline compared to healthy controls. Additionally, HO-1 levels were significantly higher in patients with septic shock compared to patients with severe sepsis. Finally, levels of HO-1 and mtDNA, but not of hemopexin, seemed to slowly revert back towards levels measured in healthy donors within 5 days after admission. Conclusions Our results indicate that plasma levels of the hemoprotein scavengers hemopexin, haptoglobin and HO-1 and the mitochondrial damage marker mtDNA might be useful as additional biomarkers for the early diagnosis of sepsis and disease severity.
机译:背景,尽管诊断,干预和支持性护理有所改善,但脓毒症患者的死亡率仍然很高。对过去十年的研究试图鉴定能够准确地区分脓毒症的生物标志物与其他疾病的败血症具有可比症状来改善诊断,但结果略有巨大。最近的研究表明,由于溶血结果,血栓蛋白和损伤相关的分子模式(潮湿),例如线粒体DNA(MTDNA)发挥了重要作用在败血症的发病机制中。本研究的目的是测量血蛋白血红蛋白,哈达氟胺和血红素氧酶-1(HO-1)的间接标志物的血浆水平以及败血症患者群体等离子体中的线粒体损伤标记MTDNA,以确定可行性他们用作败血症诊断中的生物标志物。方法通过ELISA和MTDNA在血浆中测量血红蛋白,哈达氟胺和HO-1,通过数字液滴PCR测量MTDNA。在32例严重脓毒症和8名脓毒症患者的患者中测量血红素,哈帕氟胺,HO-1和MTDNA的血浆水平,并在基线的脓毒症休克和入院后4天和20例健康供体。结果血红素素血浆水平显着降低,HO-1的血浆水平,与健康对照相比,基线严重脓毒症和脓毒症休克的患者显着高。此外,与患有严重败血症患者相比,脓毒症患者的HO-1水平显着高。最后,HO-1和MTDNA的水平,但不含血红蛋白,似乎在入院后5天内缓慢恢复为在健康供体中测量的水平。结论我们的结果表明,血蛋白清除剂血红蛋白,哈达氟胺和HO-1的血浆水平和线粒体损伤标志物MTDNA可能是用于早期诊断脓毒症和疾病严重程度的额外生物标志物。

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