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有机酸混合物正在利用宿主诱导型一氧化氮合酶和一氧化氮来减少体外感染。

Blends of Organic Acids Are Weaponizing the Host iNOS and Nitric Oxide to Reduce Infection of in vitro.

作者信息

Corcionivoschi Nicolae, Balta Igori, McCleery David, Pet Ioan, Iancu Tiberiu, Julean Calin, Marcu Adela, Stef Lavinia, Morariu Sorin

机构信息

Bacteriology Branch, Veterinary Sciences Division, Agri-Food and Biosciences Institute, Belfast BT4 3SD, Northern Ireland, UK.

Faculty of Bioengineering of Animal Resources, University of Life Sciences King Mihai I from Timisoara, 300645 Timisoara, Romania.

出版信息

Antioxidants (Basel). 2024 Apr 28;13(5):542. doi: 10.3390/antiox13050542.

Abstract

For the last 30 years, has caused major economic losses to the aquaculture industry as the aetiological agent for the piscirickettsiosis disease. Replacing the current interventions, based on antibiotics, with natural alternatives (e.g., organic acids) represents a priority. With this study, we aimed to better understand their biological mechanism of action in an in vitro model of infection with salmon epithelial cells (CHSE-214). Our first observation revealed that at the sub-inhibitory concentration of 0.5%, the organic acid blend (Aq) protected epithelial cell integrity and significantly reduced invasion. The MIC was established at 1% Aq and the MBC at 2% against . The sub-inhibitory concentration significantly increased the expression of the antimicrobial peptides Cath2 and Hepcidin1, and stimulated the activity of the innate immune effector iNOS. The increase in iNOS activity also led to higher levels of nitric oxide (NO) being released in the extracellular space. The exposure of to the endogenous NO caused an increase in bacterial lipid peroxidation levels, a damaging effect which can ultimately reduce the pathogen's ability to attach or multiply intracellularly. We also demonstrate that the increased NO release by the host CHSE-214 cells is a consequence of direct exposure to Aq and is not dependent on infection. Additionally, the presence of Aq during infection of CHSE-214 cells significantly mitigated the expression of the pro-inflammatory cytokines IL-1β, IL-8, IL-12, and IFNγ. Taken together, these results indicate that, unlike antibiotics, natural antimicrobials can weaponize the iNOS pathway and secreted nitric oxide to reduce infection and inflammation in a in vitro model of infection.

摘要

在过去30年里,作为鱼类立克次氏体病的病原体,给水产养殖业造成了重大经济损失。用天然替代品(如有机酸)取代目前基于抗生素的干预措施是当务之急。通过这项研究,我们旨在更好地了解它们在鲑鱼上皮细胞(CHSE-214)感染的体外模型中的生物学作用机制。我们的首次观察表明,在0.5%的亚抑制浓度下,有机酸混合物(Aq)可保护上皮细胞的完整性,并显著减少(病原体名称未给出,原文此处缺失关键信息)的侵袭。针对(病原体名称未给出,原文此处缺失关键信息),确定的最低抑菌浓度为1%的Aq,最低杀菌浓度为2%。亚抑制浓度显著增加了抗菌肽Cath2和铁调素1的表达,并刺激了先天性免疫效应因子诱导型一氧化氮合酶(iNOS)的活性。iNOS活性的增加还导致细胞外空间释放更高水平的一氧化氮(NO)。(病原体名称未给出,原文此处缺失关键信息)暴露于内源性NO导致细菌脂质过氧化水平增加,这是一种破坏性作用,最终可降低病原体在细胞内附着或繁殖的能力。我们还证明,宿主CHSE-214细胞释放的NO增加是直接暴露于Aq的结果,而不依赖于(病原体名称未给出,原文此处缺失关键信息)感染。此外,在CHSE-214细胞感染(病原体名称未给出,原文此处缺失关键信息)期间,Aq的存在显著减轻了促炎细胞因子IL-1β、IL-8、IL-12和IFNγ的表达。综上所述,这些结果表明,与抗生素不同,天然抗菌剂可以利用iNOS途径和分泌的一氧化氮来减少体外感染模型中的感染和炎症。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fbe7/11118739/03d6e429aa7c/antioxidants-13-00542-g001.jpg

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