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Beta-Defensin-2 and Beta-Defensin-3 Reduce Intestinal Damage Caused by Salmonella typhimurium Modulating the Expression of Cytokines and Enhancing the Probiotic Activity of Enterococcus faecium

机译:β-防御素2和β-防御素3减少了鼠伤寒沙门氏菌对细胞因子表达的调节并增强了粪肠球菌的益生菌活性而引起的肠道损伤。

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摘要

The intestinal microbiota is a major factor in human health and disease. This microbial community includes autochthonous (permanent inhabitants) and allochthonous (transient inhabitants) microorganisms that contribute to maintaining the integrity of the intestinal wall, modulating responses to pathogenic noxae and representing a key factor in the maturation of the immune system. If this healthy microbiota is disrupted by antibiotics, chemotherapy, or a change in diet, intestinal colonization by pathogenic bacteria or viruses may occur, leading to disease. To manage substantial microbial exposure, epithelial surfaces of the intestinal tract produce a diverse arsenal of antimicrobial peptides (AMPs), including, of considerable importance, the β-defensins, which directly kill or inhibit the growth of microorganisms. Based on the literature data, the purpose of this work was to create a line of intestinal epithelial cells able to stably express gene encoding human β-defensin-2 (hBD-2) and human β-defensin-3 (hBD-3), in order to test their role in S. typhimurium infections and their interaction with the bacteria of the gut microbiota.
机译:肠道菌群是人类健康和疾病的主要因素。该微生物群落包括有助于维持肠壁完整性,调节对致病性诺曼氏菌的反应并代表免疫系统成熟的关键因素的自生(永久居民)和异源(暂时居民)微生物。如果这种健康的微生物群被抗生素,化学疗法或饮食改变所破坏,则可能会发生由病原菌或病毒引起的肠道定植,从而导致疾病。为了控制大量的微生物暴露,肠道的上皮表面会产生多种抗菌肽(AMPs),其中包括非常重要的β-防御素,它们会直接杀死或抑制微生物的生长。根据文献数据,这项工作的目的是创建一系列能够稳定表达编码人β-防御素2(hBD-2)和人β-防御素3(hBD-3)的基因的肠上皮细胞,为了测试它们在鼠伤寒沙门氏菌感染中的作用以及它们与肠道菌群细菌的相互作用。

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