Towards the human intestinal microbiota phylogenetic core

Tap, Julien; Mondot, Stanislas; Levenez, Florence; Pelletier, Éric; Caron, Christophe; Furet, Jean-Pierre; Ugarte, Edgardo; Muñoz-Tamayo, Rafael; Paslier, Denis Le; Nalin, Renaud; Doré, Joël; Leclerc, Marion

doi:10.1111/j.1462-2920.2009.01982.x

Cited by 773 publications

(582 citation statements)

References 48 publications

(69 reference statements)

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“…The core microbiota has been taken to mean those components (taxa or genes) common to all or the vast majority of humans (18), although others have used the term simply to mean those taxa present in a majority of their subjects (19). The incomplete characterization of these complex communities must be acknowledged when addressing questions about the core microbiota and especially, its absence (1); the problems are exacerbated if complete characterization requires sampling an individual over time.…”

Section: Discussionmentioning

confidence: 99%

Incomplete recovery and individualized responses of the human distal gut microbiota to repeated antibiotic perturbation

Dethlefsen

Relman

2010

Proc. Natl. Acad. Sci. U.S.A.

1,919

1,575

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The indigenous human microbiota is essential to the health of the host. Although the microbiota can be affected by many features of modern life, we know little about its responses to disturbance, especially repeated disturbances, and how these changes compare with baseline temporal variation. We examined the distal gut microbiota of three individuals over 10 mo that spanned two courses of the antibiotic ciprofloxacin, analyzing more than 1.7 million bacterial 16S rRNA hypervariable region sequences from 52 to 56 samples per subject. Interindividual variation was the major source of variability between samples. Day-to-day temporal variability was evident but constrained around an average community composition that was stable over several months in the absence of deliberate perturbation. The effect of ciprofloxacin on the gut microbiota was profound and rapid, with a loss of diversity and a shift in community composition occurring within 3–4 d of drug initiation. By 1 wk after the end of each course, communities began to return to their initial state, but the return was often incomplete. Although broadly similar, community changes after ciprofloxacin varied among subjects and between the two courses within subjects. In all subjects, the composition of the gut microbiota stabilized by the end of the experiment but was altered from its initial state. As with other ecosystems, the human distal gut microbiome at baseline is a dynamic regimen with a stable average state. Antibiotic perturbation may cause a shift to an alternative stable state, the full consequences of which remain unknown.

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Section: Discussionmentioning

confidence: 99%

Incomplete recovery and individualized responses of the human distal gut microbiota to repeated antibiotic perturbation

Dethlefsen

Relman

2010

Proc. Natl. Acad. Sci. U.S.A.

1,919

1,575

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“…The human GI-tract, although harbouring a vast number of microbes, has only a limited diversity at the phylum level. Microbes from seven bacterial phyla (Firmicutes, Bacteroidetes, Actinobacteria, Proteobacteria, Fusobacteria, Verromicrobia and Cyanobacteria-like) and one archael phylum (Euryarchaeota) have been detected in the human intestine (17)(18)(19)(20)(21) . However, the majority of the GI-tract population are representatives of three phyla: the Firmicutes (Families Lachnospiraceae and Ruminococcaceae), the Bacteroidetes (Bacteroidaceae, Prevotellaceae and Rikenellaceae) and the Actinobacteria (Bifidobacteriaceae and Coriobacteriaceae).…”

Section: Human Gut Microbiotamentioning

confidence: 99%

Human gut microbiota: does diet matter?

2014

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The human oro-gastrointestinal (GI) tract is a complex system, consisting of oral cavity, pharynx, oesophagus, stomach, small intestine, large intestine, rectum and anus, which all together with the accessory digestive organs constitute the digestive system. The function of the digestive system is to break down dietary constituents into small molecules and then absorb these for subsequent distribution throughout the body. Besides digestion and carbohydrate metabolism, the indigenous microbiota has an important influence on host physiological, nutritional and immunological processes, and commensal bacteria are able to modulate the expression of host genes that regulate diverse and fundamental physiological functions. The main external factors that can affect the composition of the microbial community in generally healthy adults include major dietary changes and antibiotic therapy. Changes in some selected bacterial groups have been observed due to controlled changes to the normal diet e.g. high-protein diet, high-fat diet, prebiotics, probiotics and polyphenols. More specifically, changes in the type and quantity of non-digestible carbohydrates in the human diet influence both the metabolic products formed in the lower regions of the GI tract and the bacterial populations detected in faeces. The interactions between dietary factors, gut microbiota and host metabolism are increasingly demonstrated to be important for maintaining homeostasis and health. Therefore the aim of this review is to summarise the effect of diet, and especially dietary interventions, on the human gut microbiota. Furthermore, the most important confounding factors (methodologies used and intrinsic human factors) in relation to gut microbiota analyses are elucidated.

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“…The species level taxonomy of this community can vary significantly between individuals but the core microbiome is conserved and has high functional redundancy. [1][2][3] The host relies on these microbial denizens for nutrition, regulation of intestinal structures, immune system development, and protection from opportunistic pathogens. [4][5][6] The microbiome plays an essential role in maintaining the host health.…”

Section: Introductionmentioning

confidence: 99%

Impact of probiotic supplements on microbiome diversity following antibiotic treatment of mice

2016

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Shifts in microbial populations of the intestinal tract have been associated with a multitude of nutritional, autoimmune, and infectious diseases. The limited diversity following antibiotic treatments creates a window for opportunistic pathogens, diarrhea, and inflammation as the microbiome repopulates. Depending on the antibiotics used, microbial diversity can take weeks to months to recover. To alleviate this loss of diversity in the intestinal microbiota, supplementation with probiotics has become increasingly popular. However, our understanding of the purported health benefits of these probiotic bacteria and their ability to shape the microbiome is significantly lacking. This study examined the impact of probiotics concurrent with antibiotic treatment or during the recovery phase following antibiotic treatment of mice. We found that probiotics did not appear to colonize the intestine themselves or shift the overall diversity of the intestinal microbiota. However, the probiotic supplementation did significantly change the types of bacteria which were present. In particular, during the recovery phase the probiotic caused a suppression of Enterobacteriaceae outgrowth (Shigella and Escherichia) while promoting a blooming of Firmicutes, particularly from the Anaerotruncus genus. These results indicate that probiotics have a significant capacity to remodel the microbiome of an individual recovering from antibiotic therapy.

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Towards the human intestinal microbiota phylogenetic core

Cited by 773 publications

References 48 publications

Incomplete recovery and individualized responses of the human distal gut microbiota to repeated antibiotic perturbation

Incomplete recovery and individualized responses of the human distal gut microbiota to repeated antibiotic perturbation

Human gut microbiota: does diet matter?

Impact of probiotic supplements on microbiome diversity following antibiotic treatment of mice

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