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In vitro batch fermentation demonstrates variations in the regulation of gut microbiota and metabolic functions by β-glucans of differing structures

糖苷键 发酵 肠道菌群 酵母 细菌 微生物代谢 生物 微生物学 食品科学 生物化学 遗传学
作者
Yuhang Gao,Leilei Yu,Zi Ye,Chuan Zhang,Yuhong Gong,Qingsong Zhang,Chengcheng Zhang,Jianxin Zhao,Arjan Narbad,Wei Chen,Qixiao Zhai,Fengwei Tian
出处
期刊:Food Research International [Elsevier]
卷期号:186: 114287-114287 被引量:3
标识
DOI:10.1016/j.foodres.2024.114287
摘要

The gut microbiota is widely acknowledged as a crucial factor in regulating host health. The structure of dietary fibers determines changes in the gut microbiota and metabolic differences resulting from their fermentation, which in turn affect gut microbe-related health effects. β-Glucan (BG) is a widely accessible dietary fiber to humans, and its structural characteristics vary depending on the source. However, the interactions between different structural BGs and gut microbiota remain unclear. This study used an in vitro fermentation model to investigate the effects of BG on gut microbiota, and microbiomics and metabolomics techniques to explore the relationship between the structure of BG, bacterial communities, and metabolic profiles. The four sources of BG (barley, yeast, algae, and microbial fermentation) contained different types and proportions of glycosidic bonds, which differentially altered the bacterial community. The BG from algal sources, which contained only β(1 → 4) glycosidic bonds, was the least metabolized by the gut microbiota and caused limited metabolic changes. The other three BGs contain more diverse glycosidic bonds and can be degraded by bacteria from multiple genera, causing a wider range of metabolic changes. This work also suggested potential synergistic degradation relationships between gut bacteria based on BG. Overall, this study deepens the structural characterization-microbial-functional understanding of BGs and provides theoretical support for the development of gut microbiota-targeted foods.
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