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使用体外模拟人体肠道微生物生态系统(SHIME)模型研究健康个体和受损个体肠道中细菌α多样性与真菌定植之间的复杂联系。

The Intricate Connection between Bacterial α-Diversity and Fungal Engraftment in the Human Gut of Healthy and Impaired Individuals as Studied Using the In Vitro SHIME Model.

作者信息

Marsaux Benoît, Moens Frédéric, Marzorati Massimo, Van de Wiele Tom

机构信息

ProDigest B.V., Technologiepark-Zwijnaarde 82, 9052 Ghent, Belgium.

Center for Microbial Ecology and Technology (CMET), Ghent University, Coupure Links 653, 9000 Ghent, Belgium.

出版信息

J Fungi (Basel). 2023 Aug 26;9(9):877. doi: 10.3390/jof9090877.

Abstract

From the estimated 2.2 to 3.8 million fungal species existing on Earth, only a minor fraction actively colonizes the human gastrointestinal tract. In fact, these fungi only represent 0.1% of the gastrointestinal biosphere. Despite their low abundance, fungi play dual roles in human health-both beneficial and detrimental. Fungal infections are often associated with bacterial dysbiosis following antibiotic use, yet our understanding of gut fungi-bacteria interactions remains limited. Here, we used the SHIME gut model to explore the colonization of human fecal-derived fungi across gastrointestinal compartments. We accounted for the high inter-individual microbial diversity by using fecal samples from healthy adults, healthy babies, and Crohn's disease patients. Using quantitative Polymerase Chain Reaction and targeted next-generation sequencing, we demonstrated that SHIME-colonized mycobiomes change upon loss of transient colonizers. In addition, SHIME reactors from Crohn's disease patients contained comparable bacterial levels as healthy adults but higher fungal concentrations, indicating unpredictable correlations between fungal levels and total bacterial counts. Our findings rather link higher bacterial α-diversity to limited fungal growth, tied to colonization resistance. Hence, while healthy individuals had fewer fungi engrafting the colonic reactors, low α-diversity in impaired (Crohn's disease patients) or immature (babies) microbiota was associated with greater fungal abundance. To validate, antibiotic-treated healthy colonic microbiomes demonstrated increased fungal colonization susceptibility, and bacterial taxa that were negatively correlated with fungal expansion were identified. In summary, fungal colonization varied individually and transiently, and bacterial resistance to fungal overgrowth was more related with specific bacterial genera than total bacterial load. This study sheds light on fungal-bacterial dynamics in the human gut.

摘要

地球上估计存在220万至380万种真菌,但只有一小部分会主动定殖于人类胃肠道。实际上,这些真菌仅占胃肠道生物群落的0.1%。尽管其丰度较低,但真菌在人类健康中发挥着双重作用——既有有益的一面,也有有害的一面。真菌感染通常与抗生素使用后导致的细菌失调有关,然而我们对肠道真菌与细菌相互作用的了解仍然有限。在这里,我们使用SHIME肠道模型来探索源自人类粪便的真菌在胃肠道各部分的定殖情况。我们通过使用来自健康成年人、健康婴儿和克罗恩病患者的粪便样本,考虑到了个体间微生物的高度多样性。通过定量聚合酶链反应和靶向新一代测序,我们证明了在短暂定殖菌消失后,SHIME定殖的真菌群落会发生变化。此外,来自克罗恩病患者的SHIME反应器中的细菌水平与健康成年人相当,但真菌浓度更高,这表明真菌水平与细菌总数之间存在不可预测的相关性。我们的研究结果表明,较高的细菌α多样性与有限的真菌生长相关,这与定殖抗性有关。因此,虽然健康个体在结肠反应器中定殖的真菌较少,但受损(克罗恩病患者)或不成熟(婴儿)的微生物群中较低的α多样性与更高的真菌丰度相关。为了进行验证,用抗生素处理过的健康结肠微生物群显示出对真菌定殖的易感性增加,并且鉴定出了与真菌扩张呈负相关的细菌分类群。总之,真菌定殖存在个体差异且是短暂的,细菌对真菌过度生长的抗性更多地与特定细菌属有关,而不是与细菌总数有关。这项研究揭示了人类肠道中真菌与细菌的动态关系。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1db0/10532570/84620194b8d6/jof-09-00877-g001.jpg

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