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鞣花酸可预防肠道损伤,改善与微生物相关的肠道淋巴细胞失衡。

Ellagic acid prevents gut damage ameliorating microbe-associated intestinal lymphocyte imbalance.

机构信息

Animal Nutritional Genome and Germplasm Innovation Research Center, College of Animal Science and Technology, Hunan Agricultural University, Changsha, Hunan 410128, China.

出版信息

Food Funct. 2022 Oct 3;13(19):9822-9831. doi: 10.1039/d2fo01512a.

Abstract

Inflammatory bowel disease (IBD) pathogenesis involves a sustained microbial-mediated immune response following intestinal stress. Although administration of antibiotics can be an effective therapy, the misuse of antibiotics may risk unknown drug-resistant bacteria. In this study, piglets pretreated with ellagic acid (EA) and Ampicillin (AMP) for 21 days, and were injected intraperitoneally with paraquat (PQ) on 14 and 18 days. We found piglets lost most of their gut microbes in the AMP group, protected from subsequent intestinal damage caused by gut oxidative stress. Hence, we identified some gut microbes that may play a critical role in mediating cellular responses following cytokine stimulation in PQ-induced stress. EA preprocessing exhibited the same performance as AMP. Pretreatment of EA reduced abundance in the gut. Particularly, EA modulated intestinal lymphocyte distribution, reduced the frequency of CD79a cells, and alleviated the upward migration of CD3 cells to the apex of the intestinal villi in the intestinal epithelium. Additionally, the intestinal immune response had been known associated closely with the abundance of in the gut. Thus, we concluded that EA has the potential to replace antibiotics to prevent microbial-mediated immune responses in the gut, and EA can be applied as a supplement candidate to alleviate the development of inflammation caused by intestinal stress.

摘要

炎症性肠病 (IBD) 的发病机制涉及肠道应激后持续的微生物介导的免疫反应。尽管抗生素的使用可以是一种有效的治疗方法,但抗生素的滥用可能会带来未知的耐药细菌风险。在这项研究中,预先用鞣花酸 (EA) 和氨苄西林 (AMP) 处理的仔猪在第 14 和 18 天经腹腔注射百草枯 (PQ)。我们发现 AMP 组的仔猪失去了大部分肠道微生物,从而免受随后由肠道氧化应激引起的肠道损伤。因此,我们确定了一些可能在 PQ 诱导的应激后细胞因子刺激介导细胞反应中发挥关键作用的肠道微生物。EA 预处理表现出与 AMP 相同的性能。EA 预处理减少了肠道中 的丰度。特别是,EA 调节了肠道淋巴细胞的分布,降低了 CD79a 细胞的频率,并减轻了 CD3 细胞向上迁移到肠绒毛顶端的现象。此外,肠道免疫反应与肠道中 的丰度密切相关。因此,我们得出结论,EA 有可能替代抗生素来预防肠道中微生物介导的免疫反应,EA 可以作为补充候选物应用,以减轻肠道应激引起的炎症发展。

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