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源自人结肠的可溶性因子可调节肠道微生物群组成。

Human colon-derived soluble factors modulate gut microbiota composition.

作者信息

Hevia Arancha, Bernardo David, Montalvillo Enrique, Al-Hassi Hafid O, Fernández-Salazar Luis, Garrote Jose A, Milani Christian, Ventura Marco, Arranz Eduardo, Knight Stella C, Margolles Abelardo, Sánchez Borja

机构信息

Department of Microbiology and Biochemistry of Dairy Products, Instituto de Productos Lácteos de Asturias - Consejo Superior de Investigaciones Científicas (IPLA-CSIC) , Villaviciosa , Spain.

Antigen Presentation Research Group, Imperial College London , Harrow , UK ; Gastroenterology Unit, Hospital Universitario de La Princesa and Instituto de Investigación Sanitaria Princesa (IIS-IP), Centro de Investigación Biomédica en Red de Enfermedades Hepáticas y Digestivas (CIBEREHD) , Madrid , Spain.

出版信息

Front Oncol. 2015 Apr 13;5:86. doi: 10.3389/fonc.2015.00086. eCollection 2015.

Abstract

The commensal microbiota modulates immunological and metabolic aspects of the intestinal mucosa contributing to development of human gut diseases including inflammatory bowel disease. The host/microbiota interaction often referred to as a crosstalk, mainly focuses on the effect of the microbiota on the host neglecting effects that the host could elicit on the commensals. Colonic microenvironments from three human healthy controls (obtained from the proximal and distal colon, both in resting conditions and after immune - IL-15- and microbiota - LPS-in vitro challenges) were used to condition a stable fecal population. Subsequent 16S rRNA gene-based analyses were performed to study the effect induced by the host on the microbiota composition and function. Non-supervised principal component analysis (PCA) showed that all microbiotas, which had been conditioned with colonic microenvironments clustered together in terms of relative microbial composition, suggesting that soluble factors were modulating a stable fecal population independently from the treatment or the origin. Our findings confirmed that the host intestinal microenvironment has the capacity to modulate the gut microbiota composition via yet unidentified soluble factors. These findings indicate that an appropriate understanding of the factors of the host mucosal microenvironment affecting microbiota composition and function could improve therapeutic manipulation of the microbiota composition.

摘要

共生微生物群调节肠道黏膜的免疫和代谢方面,这对包括炎症性肠病在内的人类肠道疾病的发展有影响。宿主/微生物群的相互作用通常被称为串扰,主要关注微生物群对宿主的影响,而忽略了宿主可能对共生菌产生的影响。来自三名健康人类对照的结肠微环境(取自近端和远端结肠,分别处于静息状态以及在体外接受免疫-IL-15和微生物群-LPS刺激后)被用于驯化稳定的粪便菌群。随后进行基于16S rRNA基因的分析,以研究宿主对微生物群组成和功能的诱导作用。非监督主成分分析(PCA)表明,所有经结肠微环境驯化的微生物群在相对微生物组成方面聚集在一起,这表明可溶性因子独立于处理方式或来源调节稳定的粪便菌群。我们的研究结果证实,宿主肠道微环境有能力通过尚未确定的可溶性因子调节肠道微生物群组成。这些发现表明,正确理解影响微生物群组成和功能的宿主黏膜微环境因素,可能会改善对微生物群组成的治疗性调控。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/914a/4394693/a1773d8aaacb/fonc-05-00086-g001.jpg

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