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手术患者实验性和临床脓毒症中内毒素释放的意义——抗生素诱导内毒素释放的证据?

The significance of endotoxin release in experimental and clinical sepsis in surgical patients--evidence for antibiotic-induced endotoxin release?

作者信息

Holzheimer R G

机构信息

Klinik für Allgemeinchirurgie, Martin-Luther-Universität Halle-Wittenberg, Germany.

出版信息

Infection. 1998 Mar-Apr;26(2):77-84. doi: 10.1007/BF02767765.

Abstract

Sepsis and peritonitis remain a serious challenge for surgical patients, despite improvement in surgical therapy and intensive care and the introduction of new powerful antibiotics. Recent in vitro studies revealed the potential of certain antibiotics, e.g. penicillin-binding protein (PBP) 3-specific antibiotics, to cause antibiotic-induced endotoxin release. Other types of antibiotics, e.g., PBP 2-specific antibiotics, were associated with no or less endotoxin release. Further in vitro experiments and investigations in animals support the hypothesis of antibiotic-induced endotoxin release, but there is little clinical evidence. The clinical significance of endotoxin is subject of open dispute with many pro's and contra's. Endotoxin, although an important trigger, may not be the only factor to induce cytokine release, e.g., peptidoglycans were able to stimulate cells to release cytokines. Gram-positive pathogens have gained more importance in clinical sepsis and may not be sufficiently reflected in current clinical studies. The hypothesis that neutralization of endotoxin and pro-inflammatory cytokines is beneficial in sepsis was seriously challenged by the results of recent clinical and experimental studies. The better understanding of mechanisms in endotoxin-induced cell activation and cell, cell-receptor and soluble receptor interactions led to new treatment options. Recent reports on the complex pathogenesis of peritonitis and the detection of pathogen-related factors with intraperitoneal immune response may have implications on clinical studies investigating the potential of new compounds and the effect of antibiotics on endotoxin release. However, only few reports are available on the clinical significance of antibiotic-induced endotoxin release, and association of endotoxin release with pathogens, mortality or alteration of physiological parameters were not observed. With regard to the particulars of these studies, e.g., a small study population or low mortality rate, mortality may not be an ideal outcome parameter for these studies. There is clinical evidence for antibiotic-induced endotoxin release. However, the need for well-designed and performed studies using newly developed monitoring devices in intensive care therapy is obvious.

摘要

尽管手术治疗、重症监护有所改进,且引入了新型强效抗生素,但脓毒症和腹膜炎对于外科手术患者而言仍是严峻挑战。近期的体外研究显示,某些抗生素(如青霉素结合蛋白(PBP)3特异性抗生素)具有引发抗生素诱导的内毒素释放的可能性。其他类型的抗生素(如PBP 2特异性抗生素)则与无内毒素释放或较少的内毒素释放相关。进一步的体外实验和动物研究支持了抗生素诱导内毒素释放的假说,但临床证据很少。内毒素的临床意义存在公开争议,有许多支持和反对的观点。内毒素虽然是一个重要的触发因素,但可能不是诱导细胞因子释放的唯一因素,例如肽聚糖能够刺激细胞释放细胞因子。革兰氏阳性病原体在临床脓毒症中变得更加重要,而目前的临床研究可能对此反映不足。内毒素和促炎细胞因子的中和在脓毒症中有益这一假说受到了近期临床和实验研究结果的严重挑战。对内毒素诱导的细胞活化以及细胞、细胞受体和可溶性受体相互作用机制的更好理解带来了新的治疗选择。近期关于腹膜炎复杂发病机制的报道以及病原体相关因素与腹膜内免疫反应的检测可能会对研究新化合物潜力以及抗生素对内毒素释放影响的临床研究产生影响。然而,关于抗生素诱导内毒素释放的临床意义的报道很少,且未观察到内毒素释放与病原体、死亡率或生理参数改变之间的关联。鉴于这些研究的具体情况(例如研究人群规模小或死亡率低),死亡率可能不是这些研究的理想结局参数。有抗生素诱导内毒素释放的临床证据。然而,显然需要在重症监护治疗中使用新开发的监测设备进行精心设计和实施的研究。

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