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木糖醇通过肠道微生物群的交叉喂养增强结肠中丙酸的合成。

Xylitol enhances synthesis of propionate in the colon via cross-feeding of gut microbiota.

机构信息

School of Food Science and Biotechnology, Zhejiang Gongshang University, Hangzhou, 310018, China.

Zhejiang Huakang Pharmaceutical Co., Ltd., Kaihua, 324302, China.

出版信息

Microbiome. 2021 Mar 18;9(1):62. doi: 10.1186/s40168-021-01029-6.

Abstract

BACKGROUND

Xylitol, a white or transparent polyol or sugar alcohol, is digestible by colonic microorganisms and promotes the proliferation of beneficial bacteria and the production of short-chain fatty acids (SCFAs), but the mechanism underlying these effects remains unknown. We studied mice fed with 0%, 2% (2.17 g/kg/day), or 5% (5.42 g/kg/day) (weight/weight) xylitol in their chow for 3 months. In addition to the in vivo digestion experiments in mice, 3% (weight/volume) (0.27 g/kg/day for a human being) xylitol was added to a colon simulation system (CDMN) for 7 days. We performed 16S rRNA sequencing, beneficial metabolism biomarker quantification, metabolome, and metatranscriptome analyses to investigate the prebiotic mechanism of xylitol. The representative bacteria related to xylitol digestion were selected for single cultivation and co-culture of two and three bacteria to explore the microbial digestion and utilization of xylitol in media with glucose, xylitol, mixed carbon sources, or no-carbon sources. Besides, the mechanisms underlying the shift in the microbial composition and SCFAs were explored in molecular contexts.

RESULTS

In both in vivo and in vitro experiments, we found that xylitol did not significantly influence the structure of the gut microbiome. However, it increased all SCFAs, especially propionate in the lumen and butyrate in the mucosa, with a shift in its corresponding bacteria in vitro. Cross-feeding, a relationship in which one organism consumes metabolites excreted by the other, was observed among Lactobacillus reuteri, Bacteroides fragilis, and Escherichia coli in the utilization of xylitol. At the molecular level, we revealed that xylitol dehydrogenase (EC 1.1.1.14), xylulokinase (EC 2.7.1.17), and xylulose phosphate isomerase (EC 5.1.3.1) were key enzymes in xylitol metabolism and were present in Bacteroides and Lachnospiraceae. Therefore, they are considered keystone bacteria in xylitol digestion. Also, xylitol affected the metabolic pathway of propionate, significantly promoting the transcription of phosphate acetyltransferase (EC 2.3.1.8) in Bifidobacterium and increasing the production of propionate.

CONCLUSIONS

Our results revealed that those key enzymes for xylitol digestion from different bacteria can together support the growth of micro-ecology, but they also enhanced the concentration of propionate, which lowered pH to restrict relative amounts of Escherichia and Staphylococcus. Based on the cross-feeding and competition among those bacteria, xylitol can dynamically balance proportions of the gut microbiome to promote enzymes related to xylitol metabolism and SCFAs. Video Abstract.

摘要

背景

木糖醇是一种白色或透明的多元醇或糖醇,可被结肠微生物消化,并促进有益细菌的增殖和短链脂肪酸(SCFAs)的产生,但这些作用的机制尚不清楚。我们研究了在饲料中分别喂食 0%、2%(2.17g/kg/天)或 5%(5.42g/kg/天)(重量/重量)木糖醇的小鼠,时间为 3 个月。除了在小鼠体内进行消化实验外,还将 3%(体积/体积)(0.27g/kg/天,人类剂量)的木糖醇添加到结肠模拟系统(CDMN)中 7 天。我们进行了 16S rRNA 测序、有益代谢生物标志物定量、代谢组学和宏转录组学分析,以研究木糖醇的益生元机制。选择与木糖醇消化相关的代表性细菌进行单一培养和两种和三种细菌的共培养,以探索在含有葡萄糖、木糖醇、混合碳源或无碳源的培养基中微生物对木糖醇的消化和利用。此外,还在分子水平上探讨了微生物组成和 SCFAs 变化的机制。

结果

在体内和体外实验中,我们发现木糖醇并没有显著影响肠道微生物组的结构。然而,它增加了所有的 SCFAs,特别是腔内的丙酸和粘膜内的丁酸盐,同时体外其对应的细菌也发生了变化。在利用木糖醇的过程中,我们观察到了一种相互喂养的关系,即一种生物体消耗另一种生物体排泄的代谢物。在分子水平上,我们揭示了木糖醇脱氢酶(EC 1.1.1.14)、木酮糖激酶(EC 2.7.1.17)和木酮糖磷酸异构酶(EC 5.1.3.1)是木糖醇代谢的关键酶,存在于拟杆菌属和lachnospiraceae。因此,它们被认为是木糖醇消化的关键细菌。此外,木糖醇还影响了丙酸的代谢途径,显著促进了双歧杆菌中磷酸乙酰转移酶(EC 2.3.1.8)的转录,增加了丙酸的产生。

结论

我们的结果表明,不同细菌中用于木糖醇消化的关键酶可以共同支持微生物生态系统的生长,但它们也提高了丙酸的浓度,从而降低 pH 值,限制了相对数量的大肠杆菌和葡萄球菌的生长。基于这些细菌之间的相互喂养和竞争,木糖醇可以动态平衡肠道微生物组的比例,促进与木糖醇代谢和 SCFAs 相关的酶的产生。视频摘要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d8d8/7977168/5ce1aa52d479/40168_2021_1029_Fig1_HTML.jpg

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