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多黏菌素在生物膜相关性感染中的临床应用。

Clinical Use of Colistin in Biofilm-Associated Infections.

机构信息

Department of Internal Medicine, Hospital Universitario 12 de Octubre, Madrid, Spain.

Department of Infectious Diseases, Hospital Universitario de Bellvitge, Barcelona, Spain.

出版信息

Adv Exp Med Biol. 2019;1145:181-195. doi: 10.1007/978-3-030-16373-0_13.

Abstract

Biofilm is an adaptive bacterial strategy whereby microorganisms become encased in a complex glycoproteic matrix. The low concentration of oxygen and nutrients in this environment leads to heterogeneous phenotypic changes in the bacteria, with antimicrobial tolerance being of paramount importance. As with other antibiotics, the activity of colistin is impaired by biofilm-embedded bacteria. Therefore, the recommendation for administering high doses in combination with a second drug, indicated for planktonic infections, remains valid in this setting. Notably, colistin has activity against metabolically inactive biofilm-embedded cells located in the inner layers of the biofilm structure. This is opposite and complementary to the activity of other antimicrobials that are able to kill metabolically active cells in the outer layers of the biofilm. Several experimental models have shown a higher activity of colistin when used in combination with other agents, and have reported that this can avoid the emergence of colistin-resistant subpopulations. Most experience of colistin in biofilm-associated infections comes from patients with cystic fibrosis, where the use of nebulized colistin allows high concentrations to reach the site of the infection. However, limited clinical experience is available in other scenarios, such as osteoarticular infections or device-related central nervous system infections caused by multi-drug resistant microorganisms. In the latter scenario, the use of intraventricular or intrathecal colistin also permits high local concentrations and good clinical results. Overall, the efficacy of intravenous colistin seems to be poor, but its association with a second antimicrobial significantly increases the response rate. Given its activity against inner bioflm-embedded cells, its possible role in combination with other antibiotics, beyond last-line therapy situations, should be further explored.

摘要

生物膜是一种适应性细菌策略,通过这种策略,微生物被包裹在复杂的糖蛋白基质中。在这种环境中,氧气和营养物质的浓度较低,导致细菌表现出异质的表型变化,其中抗菌药物耐受性至关重要。与其他抗生素一样,粘菌素的活性也会被嵌入生物膜的细菌所抑制。因此,在这种情况下,建议联合使用高剂量的粘菌素和第二种针对浮游感染的药物。值得注意的是,粘菌素对位于生物膜结构内层的代谢不活跃的嵌入细胞具有活性。这与其他能够杀死生物膜外层代谢活跃细胞的抗菌药物的活性相反且互补。几个实验模型表明,粘菌素与其他药物联合使用时具有更高的活性,并且报告称这可以避免粘菌素耐药亚群的出现。在与生物膜相关的感染中,关于粘菌素的大多数经验来自囊性纤维化患者,其中使用雾化粘菌素可以使高浓度药物到达感染部位。然而,在其他情况下,如骨关节炎感染或由多药耐药微生物引起的与器械相关的中枢神经系统感染,临床经验有限。在后一种情况下,使用脑室内或鞘内粘菌素也可以达到高局部浓度并获得良好的临床效果。总体而言,静脉内粘菌素的疗效似乎较差,但与第二种抗菌药物联合使用可显著提高反应率。鉴于其对内部嵌入细胞的活性,它在联合其他抗生素(不仅仅是作为最后一线治疗药物)方面的可能作用应该进一步探索。

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