4.8 Article

Population-level analysis of gut microbiome variation

期刊

SCIENCE
卷 352, 期 6285, 页码 560-564

出版社

AMER ASSOC ADVANCEMENT SCIENCE
DOI: 10.1126/science.aad3503

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资金

  1. Flemish government [531130359]
  2. Research Fund Flanders (FWO) [G.0924.09]
  3. King Baudouin Foundation [2012-J80000-004]
  4. VIB
  5. Rega institute for Medical Research
  6. KU Leuven
  7. Agency for Innovation by Science and Technology (IWT)
  8. Marie Curie Actions FP7 People COFUND [267139]
  9. FWO
  10. Top institiute Food and Nutrition [HEN GH001]
  11. CardioVasculair Onderzoek Nederland [CVON 2012-03]
  12. Netherlands Organization for Scientific Research [NWO-VIDI 864.13.013]
  13. FP7 ERC Advanced Grant [2012-322698]
  14. [FP7 METACARDIS HEALTH-F4-2012-305312]

向作者/读者索取更多资源

Fecal microbiome variation in the average, healthy population has remained under-investigated. Here, we analyzed two independent, extensively phenotyped cohorts: the Belgian Flemish Gut Flora Project (FGFP; discovery cohort; N = 1106) and the Dutch LifeLines-DEEP study (LLDeep; replication; N = 1135). Integration with global data sets (N combined = 3948) revealed a 14-genera core microbiota, but the 664 identified genera still underexplore total gut diversity. Sixty-nine clinical and questionnaire-based covariates were found associated to microbiota compositional variation with a 92% replication rate. Stool consistency showed the largest effect size, whereas medication explained largest total variance and interacted with other covariate-microbiota associations. Early-life events such as birth mode were not reflected in adult microbiota composition. Finally, we found that proposed disease marker genera associated to host covariates, urging inclusion of the latter in study design.

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