Intestinal Microbiota in Healthy Adults: Temporal Analysis Reveals Individual and Common Core and Relation to Intestinal Symptoms

Jalanka, Jonna; Salonen, Anne; Nikkilä, Janne; Immonen, Outi; Kekkonen, Riina A.; Lahti, Leo; Palva, Airi; Vos, Willem M. de

doi:10.1371/journal.pone.0023035

Cited by 301 publications

(269 citation statements)

References 69 publications

Supporting

Mentioning

247

Contrasting

Unclassified

Order By: Relevance

“…However, cluster 5 also contained healthy subgingival samples, indicating that further investigations are necessary to understand and to develop prediction markers for chronic periodontitis. A core community (genera present in at least 50% of the samples) is usually identified in publications and provides a basis for disease diagnosis, prevention, and therapeutic targets (18,19). However, the variability of genera expands as the sample size increases, thus limiting its use for establishing an easy microbiological marker for dysbiosis.…”

Section: Discussionmentioning

confidence: 99%

Signature of Microbial Dysbiosis in Periodontitis

Meuric

Gall‐David

Boyer

et al. 2017

Appl Environ Microbiol

View full text Add to dashboard Cite

Periodontitis is driven by disproportionate host inflammatory immune responses induced by an imbalance in the composition of oral bacteria; this instigates microbial dysbiosis, along with failed resolution of the chronic destructive inflammation. The objectives of this study were to identify microbial signatures for health and chronic periodontitis at the genus level and to propose a model of dysbiosis, including the calculation of bacterial ratios. Published sequencing data obtained from several different studies (196 subgingival samples from patients with chronic periodontitis and 422 subgingival samples from healthy subjects) were pooled and subjected to a new microbiota analysis using the same Visualization and Analysis of Microbial Population Structures (VAMPS) pipeline, to identify microbiota specific to health and disease. Microbiota were visualized using CoNet and Cytoscape. Dysbiosis ratios, defined as the percentage of genera associated with disease relative to the percentage of genera associated with health, were calculated to distinguish disease from health. Correlations between the proposed dysbiosis ratio and the periodontal pocket depth were tested with a different set of data obtained from a recent study, to confirm the relevance of the ratio as a potential indicator of dysbiosis. Beta diversity showed significant clustering of periodontitis-associated microbiota, at the genus level, according to the clinical status and independent of the methods used. Specific genera (Veillonella, Neisseria, Rothia, Corynebacterium, and Actinomyces) were highly prevalent (Ͼ95%) in health, while other genera (Eubacterium, Campylobacter, Treponema, and Tannerella) were associated with chronic periodontitis. The calculation of dysbiosis ratios based on the relative abundance of the genera found in health versus periodontitis was tested. Nonperiodontitis samples were significantly identifiable by low ratios, compared to chronic periodontitis samples. When applied to a subgingival sample set with well-defined clinical data, the method showed a strong correlation between the dysbiosis ratio, as well as a simplified ratio (Porphyromonas, Treponema, and Tannerella to Rothia and Corynebacterium), and pocket depth. Microbial analysis of chronic periodontitis can be correlated with the pocket depth through specific signatures for microbial dysbiosis.IMPORTANCE Defining microbiota typical of oral health or chronic periodontitis is difficult. The evaluation of periodontal disease is currently based on probing of the periodontal pocket. However, the status of pockets "on the mend" or sulci at risk of periodontitis cannot be addressed solely through pocket depth measurements or current microbiological tests available for practitioners. Thus, a more specific microbiological measure of dysbiosis could help in future diagnoses of periodontitis. In this work, data from different studies were pooled, to improve the accuracy of the results. However, analysis of multiple species from different studies intensified the bacteri...

show abstract

Section: Discussionmentioning

confidence: 99%

Signature of Microbial Dysbiosis in Periodontitis

Meuric

Gall‐David

Boyer

et al. 2017

Appl Environ Microbiol

View full text Add to dashboard Cite

show abstract

“…literature, no consensus on a general human GI microbial core has emerged (Hamady and Knight, 2009;Tap et al, 2009;Turnbaugh et al, 2009;Qin et al, 2010;Claesson et al, 2011;Jalanka-Tuovinen et al, 2011;Salonen et al, 2012). In our cohort we could define a general core microbiota of 96 phylotype-like groups prevalent in all subjects that accounts for 34.7% of the total microbiota (s.d.…”

Section: Uncultured Clostridiales I Uncultured Clostridiales Iimentioning

confidence: 99%

“…Previous studies have shown that GI microbiota is host-specific and GI tract region-specific (Zoetendal et al, 2004;Rajilic-Stojanovic et al, 2009;Jalanka-Tuovinen et al, 2011), aberrant in composition and stability in patients suffering from GI disorders such as Crohn's disease (Seksik et al, 2003), and associated to host energy homeostasis (Backhed et al, 2004;Ley et al, 2006;Turnbaugh et al, 2006;Backhed et al, 2007;Samuel et al, 2008). Analysis of global fecal microbiomes introduced the concept that human GI microbiota appeared to have three distinct structural biometypes called enterotypes (Arumugam et al, 2011).…”

Section: Introductionmentioning

confidence: 99%

Microbiota conservation and BMI signatures in adult monozygotic twins

et al. 2012

View full text Add to dashboard Cite

The human gastrointestinal (GI) tract microbiota acts like a virtual organ and is suggested to be of great importance in human energy balance and weight control. This study included 40 monozygotic (MZ) twin pairs to investigate the influence of the human genotype on GI microbiota structure as well as microbial signatures for differences in body mass index (BMI). Phylogenetic microarraying based on 16S rRNA genes demonstrated that MZ twins have more similar microbiotas compared with unrelated subjects (Po0.001), which allowed the identification of 35 genus-like microbial groups that are more conserved between MZ twins. Half of the twin pairs were selected on discordance in terms of BMI, which revealed an inverse correlation between Clostridium cluster IV diversity and BMI. Furthermore, relatives of Eubacterium ventriosum and Roseburia intestinalis were positively correlated to BMI differences, and relatives of Oscillospira guillermondii were negatively correlated to BMI differences. Lower BMI was associated with a more abundant network of primary fiber degraders, while a network of butyrate producers was more prominent in subjects with higher BMI. Combined with higher butyrate and valerate contents in the fecal matter of higher BMI subjects, the difference in microbial networks suggests a shift in fermentation patterns at the end of the colon, which could affect human energy homeostasis.

show abstract

“…In contrast, the gut microbiota of healthy adults is individual specific and relatively stable in time (Claesson et al, 2011;Jalanka-Tuovinen et al, 2011;Rajilić-Stojanović et al, 2013). Two main phyla, Firmicutes and Bacteroidetes, constitute over 90% of the microbiota in healthy adults, followed by Actinobacteria, Proteobacteria and Verrucomicrobia (Claesson et al, 2011;Jalanka-Tuovinen et al, 2011;RingelKulka et al, 2013;Voreades et al, 2014).…”

Section: Introductionmentioning

confidence: 99%

Discordant temporal development of bacterial phyla and the emergence of core in the fecal microbiota of young children

et al. 2015

View full text Add to dashboard Cite

The colonization pattern of intestinal microbiota during childhood may impact health later in life, but children older than 1 year are poorly studied. We followed healthy children aged 1-4 years (n = 28) for up to 12 months, during which a synbiotic intervention and occasional antibiotics intake occurred, and compared them with adults from the same region. Microbiota was quantified with the HITChip phylogenetic microarray and analyzed with linear mixed effects model and other statistical approaches. Synbiotic administration increased the stability of Actinobacteria and antibiotics decreased Clostridium cluster XIVa abundance. Bacterial diversity did not increase in 1-to 5-year-old children and remained significantly lower than in adults. Actinobacteria, Bacilli and Clostridium cluster IV retained child-like abundances, whereas some other groups were converting to adult-like profiles. Microbiota stability increased, with Bacteroidetes being the main contributor. The common core of microbiota in children increased with age from 18 to 25 highly abundant genus-level taxa, including several butyrate-producing organisms, and developed toward an adult-like composition. In conclusion, intestinal microbiota is not established before 5 years of age and diversity, core microbiota and different taxa are still developing toward adult-type configuration. Discordant development patterns of bacterial phyla may reflect physiological development steps in children.

show abstract

Intestinal Microbiota in Healthy Adults: Temporal Analysis Reveals Individual and Common Core and Relation to Intestinal Symptoms

Cited by 301 publications

References 69 publications

Signature of Microbial Dysbiosis in Periodontitis

Signature of Microbial Dysbiosis in Periodontitis

Microbiota conservation and BMI signatures in adult monozygotic twins

Discordant temporal development of bacterial phyla and the emergence of core in the fecal microbiota of young children

Contact Info

Product

Resources

About