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地红霉素或其代谢产物红霉胺与氧化性多形核细胞代谢之间的体外相互作用。

In vitro interaction between dirithromycin or its metabolite, erythromycylamine, and oxidative polymorphonuclear metabolism.

作者信息

Moutard I, Gressier B, Brunet C, Dine T, Luyckx M, Cazin M, Cazin J C

机构信息

Laboratoire de Pharmacologie et Pharmacie Clinique, Faculté des Sciences Pharmaceutiques et Biologiques, Lille, France.

出版信息

J Antibiot (Tokyo). 1997 Jan;50(1):53-7. doi: 10.7164/antibiotics.50.53.

Abstract

The direct stimulation by neutrophil-infectious bacteria induces an increase in the production of reactive oxygen species which is an important host defense mechanism. Antibiotics that enter rapidly and are concentrated in neutrophils, can stimulate or damage this function. In this study, an in vitro evaluation has been made of the macrolide, dirithromycin, and its active metabolite, erythromycylamine, on the superoxide anion generation by neutrophils in three systems of stimulation: the oligopeptide fMLP, an analogue of bacterial chemotactic factors; the phorbol ester PMA, a direct activator of protein kinase C; and a bacteria strain, Staphylococcus aureus. It has been demonstrated that dirithromycin, at therapeutic plasma concentrations, and its active metabolite have a significant pro-oxidant effect on the two systems: fMLP and bacteria. This effect is greater for dirithromycin than that for erythromycylamine. At higher non-therapeutic concentrations, these substances decrease superoxide generation in the three systems. The effects of these two agents seem to be the result of an intracellular mechanism resulting in the intervention of the oxidative metabolism of neutrophils since no effect was found in the cell-free systems. Therefore, this in vitro study suggests that at therapeutic concentrations, dirithromycin and erythromycylamine could benefit therapy by stimulation of the oxidative metabolism of neutrophils.

摘要

中性粒细胞感染细菌的直接刺激会导致活性氧生成增加,这是一种重要的宿主防御机制。快速进入并集中在中性粒细胞中的抗生素会刺激或损害这一功能。在本研究中,已在三种刺激系统中对大环内酯类药物地红霉素及其活性代谢产物红霉素胺对中性粒细胞超氧阴离子生成的影响进行了体外评估:寡肽fMLP(一种细菌趋化因子类似物)、佛波酯PMA(蛋白激酶C的直接激活剂)以及一株金黄色葡萄球菌。结果表明,在治疗性血浆浓度下,地红霉素及其活性代谢产物对fMLP和细菌这两种刺激系统具有显著的促氧化作用。地红霉素的这种作用比红霉素胺更强。在高于治疗浓度时,这些物质会降低三种刺激系统中的超氧阴离子生成。这两种药物的作用似乎是一种细胞内机制的结果,导致中性粒细胞氧化代谢的干预,因为在无细胞系统中未发现任何作用。因此,这项体外研究表明,在治疗浓度下,地红霉素和红霉素胺可能通过刺激中性粒细胞的氧化代谢而有益于治疗。

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