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基于多种细菌的直接添加型微生物制剂可缓解沙门氏菌感染,维持体外肠上皮完整性。

A multispecies bacterial-based direct-fed microbial alleviates Salmonella invasion and supports in vitro epithelial integrity.

机构信息

Novonesis, Planetary Health & Biosolutions, Hørsholm 2970, Denmark.

出版信息

J Anim Sci. 2024 Jan 3;102. doi: 10.1093/jas/skae304.

Abstract

Managing bacterial infections is of great importance in livestock production, particularly those caused by Salmonella enterica serovars Typhimurium or Dublin, which can impact both animal health and performance, as well as human food safety. Direct-fed microbials (DFM) can support gastrointestinal function and alleviate the potential negative effects of bacterial infections. In the present study, the capacity of a multispecies bacterial-based DFM containing Ligilactobacillus (formerly Lactobacillus) animalis 506, Propionibacterium freudenreichii 507, Bacillus licheniformis 809, and B. subtilis 597 to reduce S. Typhimurium ATCC14028 invasion was investigated using a co-incubation model with the HT29-MTX-E12 cell line (experiment 1). Next, a possible antagonistic effect of the DFM against S. Dublin ATCC 41286 was evaluated using an in vitro agar well diffusion method following a co-incubation of 48 h (experiment 2). At last, a series of experiments were performed to evaluate how different doses (6.25 × 106, 2.50 × 107, or 1.00 × 108 CFU/well) of the DFM would support the integrity of intestinal epithelial cells challenged or not with S. Typhimurium ATCC14028 or hydrogen peroxide under a transepithelial electrical resistance (TEER) assay with Caco-2 cells (experiments 3 and 4). In experiment 1, BDP significantly (P < 0.001) reduced by 90.8% the invasion of S. Typhimurium into HT29-MTX-E12 cells, whereas viability of the potentially harmful bacteria was reduced by 21.0% (P < 0.0001). In experiment 2, the antagonistic properties of BDP towards S. Dublin were confirmed by the detection of a clear inhibition zone (size = 8.6 mm). Lastly, without challenge, the lowest dose of the DFM (6.25 × 106 CFU) provided the greatest support to the cells (treatment × hour; P < 0.0001). However, when the cells were challenged with S. Typhimurium, all doses alleviated the loss of integrity caused by the pathogen (treatment × hour; P < 0.0001). In cells challenged with hydrogen peroxide, the greater dose (1.00 × 108 CFU) supported the cells for a longer period of time (treatment × hour; P < 0.0001). These in vitro findings set the stage for exploring the potential benefits of using a novel DFM as a promising tool and strategy to mitigate S. enterica infections in ruminants and improve animal health, food safety, and public health. Further, in vivo confirmation needs to be developed to validate these preliminary in vitro results.

摘要

在畜牧业生产中,管理细菌感染非常重要,特别是由肠炎沙门氏菌血清型 Typhimurium 或都柏林引起的感染,这些感染会影响动物的健康和性能,以及人类的食品安全。直接饲喂微生物(DFM)可以支持胃肠道功能,并减轻细菌感染的潜在负面影响。在本研究中,使用包含乳杆菌(现更名为动物乳杆菌)506、丙酸杆菌 507、地衣芽孢杆菌 809 和枯草芽孢杆菌 597 的多物种细菌基 DFM 减少肠炎沙门氏菌 ATCC14028 侵袭的能力通过与 HT29-MTX-E12 细胞系共孵育模型进行了研究(实验 1)。接下来,使用体外琼脂孔扩散法评估 DFM 对肠炎沙门氏菌 ATCC 41286 的可能拮抗作用,共孵育 48 小时(实验 2)。最后,通过 Caco-2 细胞跨上皮电阻(TEER)测定,进行了一系列实验来评估 DFM 的不同剂量(6.25×106、2.50×107 或 1.00×108 CFU/孔)如何在不挑战或挑战肠炎沙门氏菌 ATCC14028 或过氧化氢的情况下支持肠上皮细胞的完整性(实验 3 和 4)。在实验 1 中,BDP 显著(P<0.001)降低了 90.8%肠炎沙门氏菌侵袭 HT29-MTX-E12 细胞的能力,而潜在有害细菌的存活率降低了 21.0%(P<0.0001)。在实验 2 中,BDP 对肠炎沙门氏菌的拮抗特性通过检测到明显的抑制区(大小=8.6mm)得到证实。最后,在没有挑战的情况下,DFM 的最低剂量(6.25×106 CFU)为细胞提供了最大的支持(处理×小时;P<0.0001)。然而,当细胞受到肠炎沙门氏菌的挑战时,所有剂量都减轻了病原体引起的完整性丧失(处理×小时;P<0.0001)。在受到过氧化氢挑战的细胞中,较大剂量(1.00×108 CFU)支持细胞的时间更长(处理×小时;P<0.0001)。这些体外发现为探索使用新型 DFM 作为减轻反刍动物肠炎沙门氏菌感染和改善动物健康、食品安全和公共卫生的有前途的工具和策略的潜在益处奠定了基础。此外,需要开发体内验证来验证这些初步的体外结果。

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