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Searching for highly sensitive and specific biomarkers for sepsis:State-of-the-art in post-mortem diagnosis of sepsis through immunohistochemicalanalysis

机译:搜索败血症的高度敏感和特异的生物标志物:通过免疫组化技术对脓毒症进行事后诊断的最新技术分析

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摘要

The autoptical observations commonly ascribed to sepsis deal with unspecific general and local signs of inflammation or ischemia, such as myocardial inflammation, pulmonary edema and infiltration, cerebral swallowing, and tubular necrosis in the kidney. In the two last decades, some studies have been carried out to implement immunohistochemical markers for post-mortem diagnosis. All of these target molecules are specifically up-regulated or down-regulated during systemic inflammatory responses, especially for infective causes. Among these, we found some antigens expressed on leukocyte surfaces (very late antigen-4 (VLA-4), cluster differentiation-15 (CD15)), enzyme contained in neutrophils granules (lysozyme (LZ), lactoferrin (LF)), endothelial markers and junctions (E-selectin, vascular endothelial cadherin (VE-cadherin)), and soluble factors (vascular endothelial growth factor (VEGF), tumor necrosis factor alpha (TNFα), procalcitonin (PCT), soluble triggering receptor expressed on myeloid cells-1 (s-TREM-1)). All of these showed potential reliability in differentiating sepsis cases from controls. Further studies are needed to provide a concrete validation for a combination of markers on specific organ samples in order to reach a post-mortem diagnosis of sepsis also in the absence of clinical records.
机译:通常归因于脓毒症的尸体观察涉及炎症或局部缺血的非特异性一般和局部体征,例如心肌炎症,肺水肿和浸润,脑吞咽和肾小管坏死。在最近的两个十年中,已经进行了一些研究以实施用于死后诊断的免疫组化标记。所有这些靶分子在全身性炎症反应期间特别是上调或下调,特别是对于感染性原因。其中,我们发现了一些在白细胞表面表达的抗原(极晚抗原4(VLA-4),簇分化15(CD15)),嗜中性粒细胞颗粒所含的酶(溶菌酶(LZ),乳铁蛋白(LF)),内皮标记和连接(E选择素,血管内皮钙粘蛋白(VE-cadherin))和可溶性因子(血管内皮生长因子(VEGF),肿瘤坏死因子α(TNFα),降钙素(PCT),在髓样细胞上表达的可溶性触发受体-1(s-TREM-1))。所有这些都表明在区分败血症病例和对照组中存在潜在的可靠性。需要进一步的研究以提供针对具体器官样品上标记物组合的具体验证,以便在缺乏临床记录的情况下也能对败血症进行事后诊断。

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