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用乙醇和丙酮酸乙酯进行预处理或后处理,会导致白细胞介素-6触发的人肺上皮细胞产生不同的抗炎反应。

Pre- or post-treatment with ethanol and ethyl pyruvate results in distinct anti-inflammatory responses of human lung epithelial cells triggered by interleukin-6.

作者信息

Relja Borna, Omid Nina, Schaible Alexander, Perl Mario, Meier Simon, Oppermann Elsie, Lehnert Mark, Marzi Ingo

机构信息

Department of Trauma, Hand and Reconstructive Surgery, University Hospital, Goethe University, Frankfurt am Main D‑60590, Germany.

Department of Trauma Surgery, Trauma Center Murnau, Murnau D‑82418, Germany.

出版信息

Mol Med Rep. 2015 Aug;12(2):2991-8. doi: 10.3892/mmr.2015.3764. Epub 2015 May 8.

Abstract

Increased local and systemic levels of interleukin (IL)-6 are associated with inflammatory processes, including neutrophil infiltration of the alveolar space, resulting in lung injury. Our previous study demonstrated the beneficial anti-inflammatory effects of acute exposure to ethanol (EtOH) in an acute in vivo model of inflammation. However, due to its side-effects, EtOH is not used clinically. In the present study, the effects of EtOH and ethyl pyruvate (EtP) as an alternative anti-inflammatory drug prior to and following application of an IL-6 stimulus on cultured A549 lung epithelial cells were compared, and it was hypothesized that treatment with EtOH and EtP reduces the inflammatory potential of the A549 cells. Time- and dose-dependent release of IL-8 from the A549 cells was observed following stimulation with IL-6. The release of IL-8 from the A549 cells was assessed following treatment with EtP (2.5-10 mM), sodium pyruvate (NaP; 10 mM) or EtOH (85-170 mM) for 1, 24 or 72 h, prior to and following IL-6 stimulation. The adhesion capacities of neutrophils to the treated A549 cells, and the expression levels of cluster of differentiation (CD)54 by the epithelial cells were measured. Treatment of the A549 cells with either EtOH or EtP significantly reduced the IL-6-induced release of IL-8. This effect was observed in the pre- and post-stimulatory conditions, which is of therapeutic importance. Similar data was revealed regarding the IL-6-induced neutrophil adhesion to the treated A549 cells, in which pre- and post-treatment with EtOH or EtP decreased the adhesion capacity, however, the results were dependent on the duration of incubation. Incubation durations of 1 and 24 h decreased the adhesion rates of neutrophils to the stimulated A549 cells, however, the reduction was only significant at 72 h post-treatment. The expression of CD54 was reduced only following treatment for 24 h with either EtOH or EtP, prior to IL-6 stimulation. Therefore, EtOH and EtP reduced the inflammatory response of lung epithelial cells, and the potential of EtP to mimic EtOH was observed in the pre- and post-treatment conditions.

摘要

白细胞介素(IL)-6的局部和全身水平升高与炎症过程相关,包括肺泡腔中性粒细胞浸润,进而导致肺损伤。我们之前的研究在急性体内炎症模型中证明了急性暴露于乙醇(EtOH)具有有益的抗炎作用。然而,由于其副作用,EtOH未在临床上使用。在本研究中,比较了在对培养的A549肺上皮细胞施加IL-6刺激之前和之后,EtOH和丙酮酸乙酯(EtP)作为替代抗炎药物的作用,并假设用EtOH和EtP处理可降低A549细胞的炎症潜能。在用IL-6刺激后,观察到A549细胞中IL-8呈时间和剂量依赖性释放。在用EtP(2.5 - 10 mM)、丙酮酸钠(NaP;10 mM)或EtOH(85 - 170 mM)处理1、24或72小时后,在IL-6刺激之前和之后,评估A549细胞中IL-8的释放。测量中性粒细胞与处理后的A549细胞的黏附能力,以及上皮细胞分化簇(CD)54的表达水平。用EtOH或EtP处理A549细胞可显著降低IL-6诱导的IL-8释放。在刺激前和刺激后的条件下均观察到这种效应,这具有治疗意义。关于IL-6诱导的中性粒细胞与处理后的A549细胞的黏附,也得到了类似的数据,其中用EtOH或EtP预处理和后处理均降低了黏附能力,然而,结果取决于孵育时间。1小时和24小时的孵育时间降低了中性粒细胞与刺激后的A549细胞的黏附率,但仅在处理后72小时降低显著。仅在用EtOH或EtP在IL-6刺激之前处理24小时后,CD54的表达才降低。因此,EtOH和EtP降低了肺上皮细胞的炎症反应,并且在预处理和后处理条件下均观察到EtP模拟EtOH的潜能。

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