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CoMiniGut—a small volume in vitro colon model for the screening of gut microbial fermentation processes

机译:CoMiniGut-用于筛选肠道微生物发酵过程的小体积体外结肠模型

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摘要

Driven by the growing recognition of the influence of the gut microbiota (GM) on human health and disease, there is a rapidly increasing interest in understanding how dietary components, pharmaceuticals and pre- and probiotics influence GM. In vitro colon models represent an attractive tool for this purpose. With the dual objective of facilitating the investigation of rare and expensive compounds, as well as an increased throughput, we have developed a prototype in vitro parallel gut microbial fermentation screening tool with a working volume of only 5 ml consisting of five parallel reactor units that can be expanded with multiples of five to increase throughput. This allows e.g., the investigation of interpersonal variations in gut microbial dynamics and the acquisition of larger data sets with enhanced statistical inference. The functionality of the in vitro colon model, Copenhagen MiniGut (CoMiniGut) was first demonstrated in experiments with two common prebiotics using the oligosaccharide inulin and the disaccharide lactulose at 1% (w/v). We then investigated fermentation of the scarce and expensive human milk oligosaccharides (HMOs) 3-Fucosyllactose, 3-Sialyllactose, 6-Sialyllactose and the more common Fructooligosaccharide in fermentations with infant gut microbial communities. Investigations of microbial community composition dynamics in the CoMiniGut reactors by MiSeq-based 16S rRNA gene amplicon high throughput sequencing showed excellent experimental reproducibility and allowed us to extract significant differences in gut microbial composition after 24 h of fermentation for all investigated substrates and fecal donors. Furthermore, short chain fatty acids (SCFAs) were quantified for all treatments and donors. Fermentations with inulin and lactulose showed that inulin leads to a microbiota dominated by obligate anaerobes, with high relative abundance of Bacteroidetes, while the more easily fermented lactulose leads to higher relative abundance of Proteobacteria. The subsequent study on the influence of HMOs on two infant GM communities, revealed the strongest bifidogenic effect for 3′SL for both infants. Inter-individual differences of infant GM, especially with regards to the occurrence of Bacteroidetes and differences in bifidobacterial species composition, correlated with varying degrees of HMO utilization foremost of 6′SL and 3′FL, indicating species and strain related differences in HMO utilization which was also reflected in SCFAs concentrations, with 3′SL and 6′SL resulting in significantly higher butyrate production compared to 3′FL. In conclusion, the increased throughput of CoMiniGut strengthens experimental conclusions through elimination of statistical interferences originating from low number of repetitions. Its small working volume moreover allows the investigation of rare and expensive bioactives.
机译:在人们越来越认识到肠道菌群(GM)对人类健康和疾病的影响的推动下,人们对理解饮食成分,药物以及益生菌和益生菌如何影响GM的兴趣迅速增长。体外结肠模型代表了用于此目的的有吸引力的工具。为了促进稀有和昂贵化合物的研究以及提高通量的双重目标,我们开发了原型体外平行肠微生物发酵筛选工具,其工作体积仅为5 ml,由五个平行反应器单元组成,以5的倍数扩展以增加吞吐量。例如,这可以研究肠道微生物动力学中的人际关系变化,并通过增强的统计推断来获取更大的数据集。体外结肠模型Copenhagen MiniGut(CoMiniGut)的功能首先在低聚糖菊粉和二糖乳果糖含量为1%(w / v)的两种常见益生元的实验中得到证实。然后,我们在婴儿肠道微生物群落的发酵中研究了稀缺且昂贵的人乳低聚糖(HMO)3-岩藻糖乳糖,3-唾液乳糖,6-唾液乳糖和更常见的低聚果糖的发酵。基于MiSeq的16S rRNA基因扩增子高通量测序对CoMiniGut反应器中微生物群落组成动态的研究显示出优异的实验可重复性,并使我们能够在发酵24小时后为所有研究的底物和粪便供体提取肠道微生物组成的显着差异。此外,对所有治疗和供体的短链脂肪酸(SCFA)进行了定量。用菊粉和乳果糖发酵表明,菊粉导致由专性厌氧菌占主导的微生物群,具有较高的拟杆菌属相对丰度,而更容易发酵的乳果糖导致较高的变形杆菌相对丰度。随后关于HMO对两个婴儿GM群落影响的研究表明,两个婴儿的3'SL的双歧化作用最强。婴儿GM的个体间差异,特别是在拟杆菌属的发生和双歧杆菌种类组成方面的差异,与6'SL和3'FL的HMO利用程度不同有关,表明物种和菌株相关的HMO利用差异SCFAs浓度也反映了这一点,与3'FL相比,3'SL和6'SL产生的丁酸明显更高。总之,通过消除源自重复次数少的统计干扰,CoMiniGut吞吐量的增加增强了实验结论。此外,它的工作量小,可以研究稀有和昂贵的生物活性物质。

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