Результаты исследований: Научные публикации в периодических изданиях › статья › Рецензирование
Population-level analysis of gut microbiome variation. / Falony, Gwen; Joossens, Marie; Vieira-Silva, Sara и др.
в: Science, Том 352, № 6285, 29.04.2016, стр. 560-564.Результаты исследований: Научные публикации в периодических изданиях › статья › Рецензирование
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TY - JOUR
T1 - Population-level analysis of gut microbiome variation
AU - Falony, Gwen
AU - Joossens, Marie
AU - Vieira-Silva, Sara
AU - Wang, Jun
AU - Darzi, Youssef
AU - Faust, Karoline
AU - Kurilshikov, Alexander
AU - Bonder, Marc Jan
AU - Valles-Colomer, Mireia
AU - Vandeputte, Doris
AU - Tito, Raul Y.
AU - Chaffron, Samuel
AU - Rymenans, Leen
AU - Verspecht, Chloë
AU - Sutter, Lise De
AU - Lima-Mendez, Gipsi
AU - D'hoe, Kevin
AU - Jonckheere, Karl
AU - Homola, Daniel
AU - Garcia, Roberto
AU - Tigchelaar, Ettje F.
AU - Eeckhaudt, Linda
AU - Fu, Jingyuan
AU - Henckaerts, Liesbet
AU - Zhernakova, Alexandra
AU - Wijmenga, Cisca
AU - Raes, Jeroen
PY - 2016/4/29
Y1 - 2016/4/29
N2 - Fecal microbiome variation in the average, healthy population has remained underinvestigated. 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.
AB - Fecal microbiome variation in the average, healthy population has remained underinvestigated. 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.
UR - http://www.scopus.com/inward/record.url?scp=84968918909&partnerID=8YFLogxK
U2 - 10.1126/science.aad3503
DO - 10.1126/science.aad3503
M3 - Article
C2 - 27126039
AN - SCOPUS:84968918909
VL - 352
SP - 560
EP - 564
JO - Science
JF - Science
SN - 0036-8075
IS - 6285
ER -
ID: 34662053