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肠道手术的常见预防性治疗方法在清除拟杆菌方面无效,而拟杆菌是全身性炎症的主要诱导因素,并且会导致小鼠在肠道屏障受损时更快死亡。

The common prophylactic therapy for bowel surgery is ineffective for clearing Bacteroidetes, the primary inducers of systemic inflammation, and causes faster death in response to intestinal barrier damage in mice.

作者信息

Sinsimer Daniel, Esseghir Amira, Tang May, Laouar Amale

机构信息

The Child Health Institute of New Jersey, Robert Wood Johnson Medical School, Rutgers University , New Brunswick, New Jersey , USA.

出版信息

BMJ Open Gastroenterol. 2015 Feb 6;1(1):e000009. doi: 10.1136/bmjgast-2014-000009. eCollection 2014.

Abstract

INTRODUCTION AND OBJECTIVE

The role of secreted gut microbial components in the initiation of systemic inflammation and consequences of antibiotic therapies on this inflammatory process are poorly elucidated. We investigate whether peripheral innate cells mount an inflammatory response to gut microbial components, the immune cells that are the primary drivers of systemic inflammation, the bacterial populations that are predominantly responsible, and whether perioperative antibiotics affect these processes.

METHOD AND EXPERIMENTAL DESIGN

Conditioned supernatants from gut microbes were used to stimulate murine innate cell types in vitro and in vivo, and proinflammatory responses were characterised. Effects of antibiotic therapies on these responses were investigated using a model of experimental intestinal barrier damage induced by dextran sodium sulfate.

RESULTS

Proinflammatory responses in the periphery are generated by components of anaerobes from the Bacteroidetes phylotype and these responses are primarily produced by myeloid dendritic cells. We found that the common prophylactic therapy for sepsis (oral neomycin and metronidazole administered to patients the day prior to surgery) is ineffective for clearing Bacteroidetes from the murine intestine. A point of critical consequence of this result is the increased systemic inflammation and premature death observed in treated mice, and these outcomes appear to be independent of gut bacterial spread in the initial phase of intestinal barrier damage. Importantly, spillage of gut microbial products, rather than dissemination of gut microbes, may underlay the initiation of systemic inflammation leading to death.

CONCLUSIONS

Our data further affirm the importance of a balanced gut microflora biodiversity in host immune homeostasis and reinforce the notion that inadequate antibiotic therapy can have detrimental effects on overall immune system.

摘要

引言与目的

肠道微生物分泌成分在全身炎症反应起始中的作用以及抗生素治疗对该炎症过程的影响尚未完全阐明。我们研究外周固有细胞是否会对肠道微生物成分产生炎症反应、作为全身炎症主要驱动因素的免疫细胞、主要负责的细菌群体,以及围手术期抗生素是否会影响这些过程。

方法与实验设计

利用肠道微生物的条件培养基上清液在体外和体内刺激小鼠固有细胞类型,并对促炎反应进行表征。使用葡聚糖硫酸钠诱导的实验性肠屏障损伤模型研究抗生素治疗对这些反应的影响。

结果

拟杆菌门厌氧菌的成分在外周引发促炎反应,这些反应主要由髓样树突状细胞产生。我们发现,败血症的常见预防性治疗方法(术前一天给患者口服新霉素和甲硝唑)对清除小鼠肠道中的拟杆菌无效。这一结果的一个关键后果是,在接受治疗(预防性用药)的小鼠中观察到全身炎症加剧和过早死亡,而且这些结果似乎与肠屏障损伤初始阶段肠道细菌的扩散无关。重要的是,肠道微生物产物的溢出而非肠道微生物的播散,可能是导致死亡的全身炎症反应起始的原因。

结论

我们的数据进一步证实了肠道微生物群生物多样性平衡在宿主免疫稳态中的重要性,并强化了抗生素治疗不当会对整体免疫系统产生有害影响的观点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/047d/4533325/7b630205e5be/bmjgast2014000009f01.jpg

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