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利奈唑胺对细菌毒素产生及宿主免疫反应的影响:证据综述

Linezolid effects on bacterial toxin production and host immune response: review of the evidence.

作者信息

Diep Binh An, Equils Ozlem, Huang David B, Gladue Ron

机构信息

Department of Medicine, University of California at San Francisco, San Francisco, California.

Medical Division, Pfizer Inc, Collegeville, Pennsylvania.

出版信息

Curr Ther Res Clin Exp. 2012 Jun;73(3):86-102. doi: 10.1016/j.curtheres.2012.04.002.

Abstract

BACKGROUND

Linezolid is active against a broad range of gram-positive pathogens and has the potential to also affect production of bacterial toxins and host immune function.

OBJECTIVE

To assess the evidence for direct effects of linezolid on bacterial toxin synthesis and modulation of host immune responses.

METHODS

Literature searches were performed of the PubMed and OVID databases. Reviews and non-English language articles were excluded. Articles with information on the effect of linezolid on bacterial toxin synthesis and immune responses were selected for further review, and data were summarized.

RESULTS

Substantial in vitro evidence supports effects of linezolid on bacterial toxin production; however, the strength of the evidence and the nature of the effects are mixed. In the case of Staphylococcus aureus, repeated observations support the inhibition of production of certain staphylococcal toxins (Panton-Valentine leukocidin, protein A, and α- and β-hemolysin) by linezolid, whereas only solitary reports indicate inhibition (toxic shock syndrome toxin-1, coagulase, autolysins, and enterotoxins A and B) or stimulation (phenol-soluble modulins) of toxin production by linezolid. In the case of Streptococcus pyogenes, there are solitary reports of linezolid inhibition (protein M, deoxyribonuclease, and streptococcal pyrogenic exotoxins A, B, and F) or stimulation (immunogenic secreted protein 2 and streptococcal inhibitor of complement-mediated lysis) of toxin production, whereas published evidence for effects on streptolysin O production is conflicting. In vitro data are limited, but suggest that linezolid might also have indirect effects on host cytokine expression through inhibition of bacterial production of toxins. In vivo data from preclinical animal studies and a single clinical study in humans are limited and equivocal insofar as a potential role for linezolid in modulating the host inflammatory response; this is due in part to the difficulty in isolating antimicrobial effects and toxin synthesis inhibitory effects of linezolid from any secondary effects on host inflammatory response.

CONCLUSIONS

Available evidence supports the possibility that linezolid can inhibit, and in some cases stimulate, toxin production in clinically relevant pathogens. However, more research will be needed to determine the potential clinical relevance of those findings for linezolid.

摘要

背景

利奈唑胺对多种革兰氏阳性病原体具有活性,并且有可能影响细菌毒素的产生和宿主免疫功能。

目的

评估利奈唑胺对细菌毒素合成和宿主免疫反应调节的直接作用的证据。

方法

对PubMed和OVID数据库进行文献检索。排除综述和非英文文章。选择有关利奈唑胺对细菌毒素合成和免疫反应影响的文章进行进一步综述,并汇总数据。

结果

大量体外证据支持利奈唑胺对细菌毒素产生的作用;然而,证据的强度和作用的性质参差不齐。就金黄色葡萄球菌而言,反复观察支持利奈唑胺抑制某些葡萄球菌毒素(杀白细胞素、蛋白A以及α和β溶血素)的产生,而仅有个别报道表明利奈唑胺抑制(中毒性休克综合征毒素-1、凝固酶、自溶素以及肠毒素A和B)或刺激(酚溶性调节蛋白)毒素的产生。就化脓性链球菌而言,有个别报道称利奈唑胺抑制(蛋白M、脱氧核糖核酸酶以及化脓性链球菌致热外毒素A、B和F)或刺激(免疫原性分泌蛋白2和补体介导溶解的链球菌抑制剂)毒素的产生,而关于其对链球菌溶血素O产生影响的已发表证据存在矛盾。体外数据有限,但提示利奈唑胺可能还通过抑制细菌毒素产生而对宿主细胞因子表达产生间接影响。临床前动物研究和一项人体临床研究的体内数据有限且不明确,无法确定利奈唑胺在调节宿主炎症反应方面的潜在作用;这部分是由于难以将利奈唑胺的抗菌作用和毒素合成抑制作用与对宿主炎症反应的任何次要作用区分开来。

结论

现有证据支持利奈唑胺能够抑制并在某些情况下刺激临床相关病原体产生毒素的可能性。然而,需要更多研究来确定这些发现对利奈唑胺的潜在临床相关性。

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