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益生菌、益生元与健康和疾病状态下的胃肠道

Probiotics, prebiotics and the gastrointestinal tract in health and disease.

作者信息

Vitetta Luis, Briskey David, Alford Hollie, Hall Sean, Coulson Samantha

机构信息

Medlab, 66 McCauley St, Alexandria, Sydney, 2015, Australia,

出版信息

Inflammopharmacology. 2014 Jun;22(3):135-54. doi: 10.1007/s10787-014-0201-4. Epub 2014 Mar 16.

Abstract

The microbiome located in the human gastrointestinal tract (GIT) comprises the largest community (diverse and dense) of bacteria, and in conjunction with a conducive internal milieu, promotes the development of regulated pro- and anti-inflammatory signals within the GIT that promotes immunological and metabolic tolerance. In addition, host-microbial interactions govern GIT inflammation and provide cues for upholding metabolic regulation in both the host and microbes. Failure to regulate inflammatory responses can increase the risk of developing inflammatory conditions in the GIT. Here, we review clinical studies regarding the efficacy of probiotics/prebiotics and the role they may have in restoring host metabolic homeostasis by rescuing the inflammatory response. The clinical studies reviewed included functional constipation, antibiotic-associated diarrhoea, Clostridium difficile diarrhoea, infectious diarrhoea/gastroenteritis, irritable bowel syndrome, inflammatory bowel diseases and necrotizing enterocolitis. We have demonstrated that there was an overall reduction in risk when probiotics were administered over placebo in the majority of GIT inflammatory conditions. The effect size of a cumulative reduction in relative risk for the GIT conditions/diseases investigated was 0.65 (0.61-0.70) (z = 13.3); p < 0.0001 that is an average reduction in risk of 35 % in favour of probiotics. We also progress a hypothesis that the GIT comprises numerous micro-axes (e.g. mucus secretion, Th1/Th2 balance) that are in operational homeostasis; hence probiotics and prebiotics may have a significant pharmacobiotic regulatory role in maintaining host GIT homeostasis in disease states partially through reactive oxygen species signalling.

摘要

位于人类胃肠道(GIT)中的微生物群是最大的细菌群落(多样且密集),在有利的内部环境作用下,可促进胃肠道内调节性促炎和抗炎信号的产生,从而促进免疫和代谢耐受。此外,宿主与微生物的相互作用控制着胃肠道炎症,并为维持宿主和微生物的代谢调节提供线索。无法调节炎症反应会增加胃肠道发生炎症性疾病的风险。在此,我们综述了关于益生菌/益生元功效的临床研究,以及它们在通过挽救炎症反应恢复宿主代谢稳态中可能发挥的作用。所综述的临床研究包括功能性便秘、抗生素相关性腹泻、艰难梭菌腹泻、感染性腹泻/肠胃炎、肠易激综合征、炎症性肠病和坏死性小肠结肠炎。我们已证明,在大多数胃肠道炎症性疾病中,使用益生菌比使用安慰剂总体风险降低。所研究的胃肠道疾病相对风险累积降低的效应大小为0.65(0.61 - 0.70)(z = 13.3);p < 0.0001,即有利于益生菌的平均风险降低35%。我们还提出了一个假设,即胃肠道包含许多处于动态平衡的微轴(如黏液分泌、Th1/Th2平衡);因此,益生菌和益生元可能在疾病状态下通过活性氧信号传导部分维持宿主胃肠道稳态方面具有重要的药物生物调节作用。

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