抗生素介导的内毒素释放和革兰氏阴性脓毒症的发病机制。

D C Morrison
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摘要

自最早使用抗生素化疗治疗革兰氏阴性微生物感染以来,研究人员已经认识到,这种治疗可能导致微生物成分的释放,进而可能加剧疾病的病理生理表现。多年来,体外研究和体内动物实验都提供了支持这一概念的证据;然而,这种现象对革兰氏阴性脓毒症患者的实际临床重要性尚不清楚。最近一些实验室发表的报告表明,细胞壁活性抗生素在破坏微生物生长方面的基本作用机制不同(通过与各种青霉素结合蛋白的选择性相互作用),在诱导生物活性内毒素释放的相对能力上也不同,无论是在体外还是体内。此外,总内毒素释放量的差异与抗生素引起的微生物形态变化密切相关。潜在的重要意义是,这些差异也反映在内毒素刺激的单核吞噬细胞和其他宿主靶细胞产生的细胞因子的差异上,包括11-6和TNF。由于这些免疫激素与革兰氏阴性脓毒症的发病机制密切相关,因此对这种化疗方法作为控制宿主免疫病理反应的手段的潜在应用的兴趣增加了。在严格对照的临床试验中,不同的抗生素治疗与细胞因子的产生相关,对于评估这种现象在革兰氏阴性脓毒症患者中的实际意义具有重要的潜在价值。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Antibiotic-mediated release of endotoxin and the pathogenesis of gram-negative sepsis.

Since the earliest days of antibiotic chemotherapy to treat infection with Gram-negative microbes, investigators have recognized that such treatments may result in the release of microbial constituents that might, in turn, exacerbate the pathophysiological manifestations of disease. Both in vitro studies and in vivo animal experiments have over the years provided evidence in support of this concept; however, the actual clinical importance of this phenomenon to patients with Gram-negative sepsis is unclear. Recently published reports from a number of laboratories have shown that cell wall-active antibiotics that differ in their fundamental mechanisms of action in disrupting microbial growth (via selective interactions with various penicillin binding proteins) also differ in their relative ability to induce the release of biologically active endotoxin both in vitro and in vivo. Further, quantitative differences in total endotoxin release correlate well with antibiotic-initiated morphological changes in the microbe. Of potential significance is the finding that these differences are also reflected in differential production of cytokines from endotoxin-stimulated mononuclear phagocytes and other host target cells, including 11-6 and TNF. Since these immunologic hormones have been strongly implicated as contributing factors to the pathogenesis of Gram-negative sepsis, interest in the potential use of this chemotherapeutic approach as a means of controlling the host immunopathologic response has increased. Carefully controlled clinical trials in which different antibiotic treatments are correlated with production of cytokines will be of significant potential value in evaluating the actual significance of this phenomenon in the Gram-negative septic patient.

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