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Dietary Modulation of Gut Microbiota Contributes to Alleviation of Both Genetic and Simple Obesity in Children()

Gut microbiota has been implicated as a pivotal contributing factor in diet-related obesity; however, its role in development of disease phenotypes in human genetic obesity such as Prader–Willi syndrome (PWS) remains elusive. In this hospitalized intervention trial with PWS (n = 17) and simple obesi...

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Autores principales: Zhang, Chenhong, Yin, Aihua, Li, Hongde, Wang, Ruirui, Wu, Guojun, Shen, Jian, Zhang, Menghui, Wang, Linghua, Hou, Yaping, Ouyang, Haimei, Zhang, Yan, Zheng, Yinan, Wang, Jicheng, Lv, Xiaofei, Wang, Yulan, Zhang, Feng, Zeng, Benhua, Li, Wenxia, Yan, Feiyan, Zhao, Yufeng, Pang, Xiaoyan, Zhang, Xiaojun, Fu, Huaqing, Chen, Feng, Zhao, Naisi, Hamaker, Bruce R., Bridgewater, Laura C., Weinkove, David, Clement, Karine, Dore, Joel, Holmes, Elaine, Xiao, Huasheng, Zhao, Guoping, Yang, Shengli, Bork, Peer, Nicholson, Jeremy K., Wei, Hong, Tang, Huiru, Zhang, Xiaozhuang, Zhao, Liping
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4563136/
https://www.ncbi.nlm.nih.gov/pubmed/26425705
http://dx.doi.org/10.1016/j.ebiom.2015.07.007
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author Zhang, Chenhong
Yin, Aihua
Li, Hongde
Wang, Ruirui
Wu, Guojun
Shen, Jian
Zhang, Menghui
Wang, Linghua
Hou, Yaping
Ouyang, Haimei
Zhang, Yan
Zheng, Yinan
Wang, Jicheng
Lv, Xiaofei
Wang, Yulan
Zhang, Feng
Zeng, Benhua
Li, Wenxia
Yan, Feiyan
Zhao, Yufeng
Pang, Xiaoyan
Zhang, Xiaojun
Fu, Huaqing
Chen, Feng
Zhao, Naisi
Hamaker, Bruce R.
Bridgewater, Laura C.
Weinkove, David
Clement, Karine
Dore, Joel
Holmes, Elaine
Xiao, Huasheng
Zhao, Guoping
Yang, Shengli
Bork, Peer
Nicholson, Jeremy K.
Wei, Hong
Tang, Huiru
Zhang, Xiaozhuang
Zhao, Liping
author_facet Zhang, Chenhong
Yin, Aihua
Li, Hongde
Wang, Ruirui
Wu, Guojun
Shen, Jian
Zhang, Menghui
Wang, Linghua
Hou, Yaping
Ouyang, Haimei
Zhang, Yan
Zheng, Yinan
Wang, Jicheng
Lv, Xiaofei
Wang, Yulan
Zhang, Feng
Zeng, Benhua
Li, Wenxia
Yan, Feiyan
Zhao, Yufeng
Pang, Xiaoyan
Zhang, Xiaojun
Fu, Huaqing
Chen, Feng
Zhao, Naisi
Hamaker, Bruce R.
Bridgewater, Laura C.
Weinkove, David
Clement, Karine
Dore, Joel
Holmes, Elaine
Xiao, Huasheng
Zhao, Guoping
Yang, Shengli
Bork, Peer
Nicholson, Jeremy K.
Wei, Hong
Tang, Huiru
Zhang, Xiaozhuang
Zhao, Liping
author_sort Zhang, Chenhong
collection PubMed
description Gut microbiota has been implicated as a pivotal contributing factor in diet-related obesity; however, its role in development of disease phenotypes in human genetic obesity such as Prader–Willi syndrome (PWS) remains elusive. In this hospitalized intervention trial with PWS (n = 17) and simple obesity (n = 21) children, a diet rich in non-digestible carbohydrates induced significant weight loss and concomitant structural changes of the gut microbiota together with reduction of serum antigen load and alleviation of inflammation. Co-abundance network analysis of 161 prevalent bacterial draft genomes assembled directly from metagenomic datasets showed relative increase of functional genome groups for acetate production from carbohydrates fermentation. NMR-based metabolomic profiling of urine showed diet-induced overall changes of host metabotypes and identified significantly reduced trimethylamine N-oxide and indoxyl sulfate, host-bacteria co-metabolites known to induce metabolic deteriorations. Specific bacterial genomes that were correlated with urine levels of these detrimental co-metabolites were found to encode enzyme genes for production of their precursors by fermentation of choline or tryptophan in the gut. When transplanted into germ-free mice, the pre-intervention gut microbiota induced higher inflammation and larger adipocytes compared with the post-intervention microbiota from the same volunteer. Our multi-omics-based systems analysis indicates a significant etiological contribution of dysbiotic gut microbiota to both genetic and simple obesity in children, implicating a potentially effective target for alleviation. RESEARCH IN CONTEXT: Poorly managed diet and genetic mutations are the two primary driving forces behind the devastating epidemic of obesity-related diseases. Lack of understanding of the molecular chain of causation between the driving forces and the disease endpoints retards progress in prevention and treatment of the diseases. We found that children genetically obese with Prader–Willi syndrome shared a similar dysbiosis in their gut microbiota with those having diet-related obesity. A diet rich in non-digestible but fermentable carbohydrates significantly promoted beneficial groups of bacteria and reduced toxin-producers, which contributes to the alleviation of metabolic deteriorations in obesity regardless of the primary driving forces.
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spelling pubmed-45631362015-09-30 Dietary Modulation of Gut Microbiota Contributes to Alleviation of Both Genetic and Simple Obesity in Children() Zhang, Chenhong Yin, Aihua Li, Hongde Wang, Ruirui Wu, Guojun Shen, Jian Zhang, Menghui Wang, Linghua Hou, Yaping Ouyang, Haimei Zhang, Yan Zheng, Yinan Wang, Jicheng Lv, Xiaofei Wang, Yulan Zhang, Feng Zeng, Benhua Li, Wenxia Yan, Feiyan Zhao, Yufeng Pang, Xiaoyan Zhang, Xiaojun Fu, Huaqing Chen, Feng Zhao, Naisi Hamaker, Bruce R. Bridgewater, Laura C. Weinkove, David Clement, Karine Dore, Joel Holmes, Elaine Xiao, Huasheng Zhao, Guoping Yang, Shengli Bork, Peer Nicholson, Jeremy K. Wei, Hong Tang, Huiru Zhang, Xiaozhuang Zhao, Liping EBioMedicine Original Article Gut microbiota has been implicated as a pivotal contributing factor in diet-related obesity; however, its role in development of disease phenotypes in human genetic obesity such as Prader–Willi syndrome (PWS) remains elusive. In this hospitalized intervention trial with PWS (n = 17) and simple obesity (n = 21) children, a diet rich in non-digestible carbohydrates induced significant weight loss and concomitant structural changes of the gut microbiota together with reduction of serum antigen load and alleviation of inflammation. Co-abundance network analysis of 161 prevalent bacterial draft genomes assembled directly from metagenomic datasets showed relative increase of functional genome groups for acetate production from carbohydrates fermentation. NMR-based metabolomic profiling of urine showed diet-induced overall changes of host metabotypes and identified significantly reduced trimethylamine N-oxide and indoxyl sulfate, host-bacteria co-metabolites known to induce metabolic deteriorations. Specific bacterial genomes that were correlated with urine levels of these detrimental co-metabolites were found to encode enzyme genes for production of their precursors by fermentation of choline or tryptophan in the gut. When transplanted into germ-free mice, the pre-intervention gut microbiota induced higher inflammation and larger adipocytes compared with the post-intervention microbiota from the same volunteer. Our multi-omics-based systems analysis indicates a significant etiological contribution of dysbiotic gut microbiota to both genetic and simple obesity in children, implicating a potentially effective target for alleviation. RESEARCH IN CONTEXT: Poorly managed diet and genetic mutations are the two primary driving forces behind the devastating epidemic of obesity-related diseases. Lack of understanding of the molecular chain of causation between the driving forces and the disease endpoints retards progress in prevention and treatment of the diseases. We found that children genetically obese with Prader–Willi syndrome shared a similar dysbiosis in their gut microbiota with those having diet-related obesity. A diet rich in non-digestible but fermentable carbohydrates significantly promoted beneficial groups of bacteria and reduced toxin-producers, which contributes to the alleviation of metabolic deteriorations in obesity regardless of the primary driving forces. Elsevier 2015-07-10 /pmc/articles/PMC4563136/ /pubmed/26425705 http://dx.doi.org/10.1016/j.ebiom.2015.07.007 Text en © 2015 The Authors http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Original Article
Zhang, Chenhong
Yin, Aihua
Li, Hongde
Wang, Ruirui
Wu, Guojun
Shen, Jian
Zhang, Menghui
Wang, Linghua
Hou, Yaping
Ouyang, Haimei
Zhang, Yan
Zheng, Yinan
Wang, Jicheng
Lv, Xiaofei
Wang, Yulan
Zhang, Feng
Zeng, Benhua
Li, Wenxia
Yan, Feiyan
Zhao, Yufeng
Pang, Xiaoyan
Zhang, Xiaojun
Fu, Huaqing
Chen, Feng
Zhao, Naisi
Hamaker, Bruce R.
Bridgewater, Laura C.
Weinkove, David
Clement, Karine
Dore, Joel
Holmes, Elaine
Xiao, Huasheng
Zhao, Guoping
Yang, Shengli
Bork, Peer
Nicholson, Jeremy K.
Wei, Hong
Tang, Huiru
Zhang, Xiaozhuang
Zhao, Liping
Dietary Modulation of Gut Microbiota Contributes to Alleviation of Both Genetic and Simple Obesity in Children()
title Dietary Modulation of Gut Microbiota Contributes to Alleviation of Both Genetic and Simple Obesity in Children()
title_full Dietary Modulation of Gut Microbiota Contributes to Alleviation of Both Genetic and Simple Obesity in Children()
title_fullStr Dietary Modulation of Gut Microbiota Contributes to Alleviation of Both Genetic and Simple Obesity in Children()
title_full_unstemmed Dietary Modulation of Gut Microbiota Contributes to Alleviation of Both Genetic and Simple Obesity in Children()
title_short Dietary Modulation of Gut Microbiota Contributes to Alleviation of Both Genetic and Simple Obesity in Children()
title_sort dietary modulation of gut microbiota contributes to alleviation of both genetic and simple obesity in children()
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4563136/
https://www.ncbi.nlm.nih.gov/pubmed/26425705
http://dx.doi.org/10.1016/j.ebiom.2015.07.007
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